Among the various methods for predicting carcinogenicity from a battery of short-term tests (STTs), the carcinogenicity prediction and battery selection (CPBS) procedure is the most prominent. A major assumption of CPBS is that the STTs used in the prediction are conditionally independent. Results of recent National Toxicology Program studies of four commonly used in vitro STTs contradict this assumption, thereby necessitating modification of CPBS to accommodate dependencies. This is accomplished via log-linear modeling, which then also yields an important dividend: standard errors for the predicted probabilities of carcinogenicity

Kim, B S

Margolin, B H

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environmentall Health Perspectives SupplementsV6l. 102 Suppl 1:127-1301994Predicting Carcinogenicity by UsingBatteries of Dependent Short-Term Testsby Byung Soo Kim' and Barry H. Margolin2Amnag the various nmehods for predictingcarcinogencity from a battery ofshort-term tests (STlb), thecarciDgenityprediction and battery selection (CPBS) procedure is the most prominent. A major ass pn ofCPBS is that the STIsused in the prediction are conditionally independent. Resultsofrecent Nationa Tlblcology Program studies offourcom-monly used in vuvSlb ona t thistsrpebon, ofCPBStocies. This is accomplished via log-linear ing, which then also yields an important dividend: standard errors for thepredicted probabilities of carcinogenicity.IntroductionCertain classes of carcinogens are poorly detected by in-dividual short-term tests (STTs). Hence, the use of a battery ofSTTs for detecting carcinogens has been recommended fiequent-ly (1-6). Several mathematical methods have been presented forprediction ofcarcinogens from batteries ofSTTs (1-3,7,8). A ma-jor assumption ofthese approaches to prediction is that STTs areconditionally independent and hence that additional STTs willallow detection of additional carcinogens.The focus here is on the carcinogenicity prediction and batteryselection (CPBS)* method, which was developed by Rosenkranzet al. (2) and applied to several known databases (4-6,9). CPBSemploys the Bayes theorem to calculate the conditional probabili-ty of carcinogenicity of a chemical given a battery of STTs. Asmentioned above, a major assumption ofCPBS is that STTs com-posing the battery are conditionally independent given the car-cinogenicity or noncarcinogenicity of the test chemical.Specifically, suppose one has a battery of r STTs, whosequalitative (positive/negative) results for a given chemical aredenoted by Al, A2, *-* Ar.Then Rosenkranz et al. (2) employedthe Bayes theorem to calculate the probability ofcarcinogenicitygiven Al, **, Aras follows:p(CA IAI A) =p(A ... Ar I CA) p(CA)p(A1* * AArI CA) p(CA) + p(AI **ArAI NC) p(NC) (1)' Department ofApplied Statistics, Yonsei University, Seoul, 120-749, SouthKorea.2 Department of Biostatistics, School ofPublic Health, Lineberger Comprehen-sive Cancer Center, University of North Carolina, CB 7400, Chapel Hill, NC27599-7400.Address reprint requests to B. S. Kim, Department ofApplied Statistics, YonseiUniversity, Seoul, 120-749, South Korea.* CPBS is a trademark of Case Western Reserve University.This paper was presented at the International Biostatistics Conference on theStudy of Toxicology that was held May 13-25, 1991, in Tokyo, Japan.They then invoked conditional independence to obtain[ P(A1 I CA) P(CA)[1 p(A i I CA)] p(CA) + [iI p(A iI NC)] p(N (2)Here CA and NC stand for carcinogenicity and noncar-cinogenicity, respectively. When A, is positive, p(Ai CA) is thesensitivity ofthe ith STT. When A, is negative, p(A, NC) is thespecificity ofthe ith STT. A similar argument can be made regar-ding p(NC Al ... Ar), the probability of noncarcinogen-icity given Al ... Ar. Equation (2) is valid only under theassumption of conditional independence of the r STTs. Thestatistical independence of several STTs has been documentedmostly by showing pairwise independence among those STTs viathe Pearson chi-square test. The analysis of published data in-dicated that about 90% ofthe pairs ofSTTs examined showed noevidence of dependence in terms of the chi-square test (1,10).This inference, however, is subject to biases of chemical and testselection plus low power to detect dependencies.In this paper, four widely used STTs are shown tobe statistical-ly dependent. The impact of this statistical dependence of thefour STTs on carcinogenicity prediction systems is explored indepth, and CPBS is extended to allow for conditionally depen-dent STTs. This permits examination of the sensitivity of car-cinogenicity predictions to the assumption of statistical in-dependence when various possible dependence structures areconsidered.DataIn 1984, the National Toxicology Program (NTP) initiated aproject with 73 chemicals to develop a database that would per-mit evaluation of the ability of four ofthe most commonly usedin vitro STTs to predict rodent carcinogenicity: the AmesKIMANDMARGOLINSalmonella/microsome mutagenicity assay (SAL), the assays forchromosome aberration (ABS) and sister chromatid exchange(SCE) induction in Chinese hamster ovary cells, and the mouselymphoma L5178Y cell mutagenesis assay [MLA (11)]. That ef-fort differed from previous investigations in two aspects (11).First, standard protocols for the four STTs were shown to yieldreproducible results in interlaboratory trials with codedchemicals. Second, the chemicals selected were those tested forcarcinogenicity by the NTP within a specified range oftime. Thisselection procedure should minimize the possibility ofchemicalselection bias.The major conclusions ofthe 73-chemical study (11) were: a)Individual qualitative concordance ofthe four STTs with rodentcarcinogenicity did not show significant differences amongassays (approximately 60%) and were much lower than previousestimates, b) there was no complementarity among STTs, and c)no battery oftests constructed from these four ST1E improved thecarcinogenicity predictivity ofthe SAL assay alone. Initial reac-tion to these conclusions withinthe genetic toxicology communitywas mixed. One of-the criticisms was that the 73 chemicals weresomewhat atypical and therefore the study needed tobe repeated.To confirm and extend the findings of Tennant et al. (11), afollow-up study was conducted for an additional 41 chemicals.The results obtained for the 41 chemicals were similar to thosereported for the 73 chemicals (12). No significant differencesbetween the two datasets were detected and hence the twodatasets were combined into a single dataset of 114. A detaileddescription of the 114-chemical data set was given in Hasemanet al. (13). The binary results of the four STTs and rodent car-cinogenicity for the 114 chemicals are in Table 3 ofHaseman etal. (13) and are reproduced here in Table 1 for analysis.MethodsThe results of the four STTs and the rodent carcinogenicity inTable 1 can be summarized in two 2 x 2 x 2 x 2 contingencytables corresponding to 67 carcinogens and 47 noncarcinogens,respectively. A log-linear analysis can be applied to these two 2x 2 x 2 x 2 contingency tables to access the dependence struc-tures of the four STTs. The log-linear model is an analysis ofvariance (ANOVA)-type data analysis method for a contingen-cy table. It represents the logarithm of expected cell frequencyas the sum of main effects of explanatory variables (STTs) andtheir interactions (14,15). The best model is selectedbased on twocompeting criteria; parsimony and goodness offit of the model.The likelihood ratio test of the SAS procedure CATMOD (16)can be used to perform the model selection. The SAS procedureCATMOD provides for each model the estimated cell frequen-cies and their standard errors. Therefore, we can evaluate p(STTresultsCA) and p(STT resultsINC) for each of the 16 possibleSTT configurations and each model considered.Following Rosenkranz, assume hat p(CA) = p(NC) = V2 forobtaining p(CAJ STT results). Application of the Bayes formulapermits calculation of the estimates of p(CAJ STT results), theprobability ofcarcinogenicity ofa chemical given its STT results,as follows:p(CAISTT results) =p(SIT resultslCA)p(CA)p(STT resultslCA)p(CA) + p(STT resultslNC)p(NC)MijklclA / 67MijklCA / 67 + MijkllC / 47 (3)where nj cA and jJNC represent estimated expected cell fre-quencies corresponding to the (ij,k,l configuration of the fourSTTs given carcinogens and noncarcinogens, respectively. Theestimated expected cell frequencies provide estimates ofp(STTresults CA) and p(STT results NC) under each possible model.Using this log-linear model approach, one can obtain estimatesAble 1. Binary results of four SiMs and rodent carcinogenicity."Carcinogenicity resultsOriginal 73 New 41 Total 114STT results chemicals chemicals chemicalsSAL ABS SCE MLA + - + - + -+ + + + 14 3 8 0 22 3+ + + -0 0 0 0 0 0+ + - + 2 0 0 0 2 0+ + -0 0 0 0 0 0+ - + + 3 1 1 0 4 1+ - + -0 0 0 0 0 0+ - - + 0 0 2 0 2 0+ - - - 1 0 1 0 2 0- + + + 5 4 3 2 8 6- + + - 2 1 0 2 2 3- + - + 0 0 0 0 0 0- + - - 1 1 0 0 1 1- - + + 5 6 2 6 7 12- - + - 3 1 0 0 3 1- - - + 2 2 1 4 3 6- - - - 6 10 5 4 11 14Total 44 29 23 18 67 47aFrom Haseman et al. (13).Abbreviations: STT, short-term test; SAL, Salmonella/microsome mutagenicity asssy; ABS, chromosome aberrations; SCE, sister chromatid exchange; MLA,mouse lymphoma L5178Y cell mutagenesis assay.128PREDICTING CARCINOGENICI7YBYDEPENDENTSHORT-TERM TESTSof p(STTI CA) and p(STT results NC) under various possible Table 2. Goodness of fit of various models.dependence structures. Hence, independence of the four STTs Carcinogens Noncarcinogensis no longer assumed. Model G2 df p G2 df pThe SAS procedure CATMOD also provides standard errors [A] [C] [M] [S] 69.93 11 0.0000 38.64 11 0.0000ofthe estimated cell frequencies. This allows us to calculate the [A] [S] [CM] 48.40 10 0.0000 22.67 10 0.0120standard errors of the estimates of p(CAI STT results) as in Equa- (SI [AC] [CM] 29.40 9 0.0006 11.17 9 0.2643[AC] [CM] [MS] 12.95 8 0.1136 6.77 5 0.2379tion 4 by using the usual 5 method. [AC] (AS] [CM] [MS] 5.69 7 0.5758 4.08 4 0.3950Var ( p(CAISTT results) ) -MCA2 mNC2- OCA2 + NC2'(MCA + mNC)4 (MCA + MNC)4whereAMCA = MijklCAAmNC = mijklINCGCA2 = [SE(A ]2i/A)I2/(67)2and (GNC2 = [SE(flijiciNC)]2/ (47)2The standard errors derived from Equation 4 make the pointestimates in Equation 3 more readily interpretable.Abbreviations: A, chromosome aberrations; C, sister chromatid exchange; M,mouse lymphoma L5178Y cell mutagenesis; S, Salmonella/microsomemutagenicity assay.conditionally independent. It is concluded here that the model[AC] [CM] [MS] is the best for both carcinogens and noncar-cinogens. The expected cell frequencies under each ofthe abovefive models are shown in Table 3.Based on the expected cell frequencies and their standarderrors (not shown) in Table 3, one can obtain estimates ofp(CAJSTT results) and their standard errors under variousmodels by using Equations (3) and (4). These estimates and stan-dard errors are shown in Table 4.DiscussionResults The observed frequencies for the positive response ofSAL andthe negativexresponse ofMLA (SAL+, MLA-) are 2 for car-Several log-linear models were fit to each ofthe two 2 x 2 x cinogens and 0 for noncarcinogens, respectively. This suggests2x 2 contingency tables. The goodness of fit ofa representative that (SAL+, MLA-) is a relatively rare event, for both car-subset of these models is shown in Table 2 in terms of the cinogens and noncarcinogens. The complete independencelikelihood ratio test statistic, G2. Following Fienberg (14) the model for the carcinogens fails to reveal this characteristic and,brackets are used to denote a model. In the brackets notation A, in general, shows substantial lack of fit in those cases where theC, M, and S stand for ABS, SCE, MLA, and SAL, respectively. STTs are in complete agreement (Table 3). The model [AC]The model [A] [C] [M] [S] is the complete independence [CM] [MS] is consistent with this observation; however, it re-model under which CPBS was developed originally. The mains to be seen whether a mechanistic interpretation can be at-goodness of fit analysis shows that the four STTs are not tached to it. In relation to the small observed frequencies forTable 3. Expected cell frequencies under various models.Carcinogens NoncarcinogensModel a Model aSAL ABS SCE MLA Observed 1 2 3 4 5 Observed 1 2 3 4 5+ + + + 22 8.2 10.2 13.6 17.8 21.9 3 0.4 0.5 0.9 1.5 2.9+ + + - 0 3.3 1.2 1.7 0.4 0.7 0 0.2 0.1 0.2 0.0 0.0+ + - + 2 3.8 1.7 0.5 0.6 1.1 0 0.3 0.1 0.0 0.0 0.1+ + - - 0 1.5 3.5 1.0 0.2 0.4 0 0.2 0.4 0.1 0.0 0.0+ - + + 4 7.5 9.4 6.0 7.8 4.8 1 1.0 1.4 1.0 1.7 0.7+ - + - 0 3.0 1.1 0.7 0.2 0.1 0 0.6 0.2 0.2 0.0 0.0+ - - + 2 3.4 1.6 2.9 3.8 2.3 0 0.8 0.4 0.5 0.8 0.3+ - - - 2 1.4 3.2 5.7 1.3 0.8 0 0.5 0.9 1.2 0.0 0.0- + + + 8 9.0 11.2 14.9 10.7 7.3 6 3.9 5.6 9.3 8.7 7.5- + + - 2 3.6 1.4 1.8 3.1 2.1 3 2.7 1.0 1.7 1.8 1.6- + - + 0 4.1 1.9 0.5 0.4 0.4 0 3.2 1.5 0.3 0.2 0.2- + - - 1 1.6 3.8 1.0 1.8 1.2 1 2.1 3.8 0.7 0.7 0.7- - + + 7 8.2 10.2 6.5 4.7 7.0 12 10.3 14.6 10.8 10.2 10.9- - + - 3 3.3 1.2 0.8 1.4 2.1 1 7.0 2.6 2.0 2.2 2.4- - - + 3 3.8 1.7 3.1 2.3 3.3 6 8.3 4.0 5.2 4.9 5.3- - - - 11 1.5 3.5 6.3 10.7 11.6 14 5.6 9.9 13.1 14.3 14.3Total 67 47Abbreviations: SAL, Salmonella/microsome mutagenicity assay (S); ABS, chromosome aberrations (A); SCE, sister chromatid exchange (C); MLA, mouse lym-phoma L5178Y cell mutagenicity assay (M).a Model 1 = [A] [C] [M] (S], model 2 = [A] [S] (CM], model 3 = (S] [AC] [CM], model 4 = [AC] [CM] [MS], model 5 = [AC] [AS] [CM] [MS].129130 KIMAND MARGOLINliable 4. Estimates of p(CAJSIT results) and their standard errors. aModelSAL ABS SCE MLA Independence [A] [S] [CM] [S] [AC] [CM] [AC] [CM] [MS]+ + + + 0.935 (0.1828) 0.933 (0.1728) 0.917 (0.1581) 0.893 (0.1426)+ + + - 0.920 (0.2223) 0.903 (0.3783) 0.881 (0.3568) 1.000 (0.8014)+ + - + 0.899 (0.2218) 0.897 (0.3197) 0.993 (0.5706) 1.000 (0.5460)+ + - - 0.840 (0.2235) 0.874 (0.2249) 0.917 (0.5032) 1.000 (0.8867)+ - + + 0.840 (0.1532) 0.829 (0.1418) 0.806 (0.1795) 0.763 (0.1588)+ - + - 0.778 (0.1646) 0.765 (0.2755) 0.736 (0.2757) 1.000 (0.8269)+ - - + 0.749 (0.1563) 0.752 (0.2299) 0.805 (0.2541) 0.769 (0.2269)+ - - - 0.663 (0.1502) 0.708 (0.1564) 0.768 (0.1699) 1.000 (0.7154)- + + + 0.618 (0.0878) 0.585 (0.0820) 0.529 (0.0778) 0.463 (0.0093)- + + - 0.483 (0.1070) 0.486 (0.1785) 0.430 (0.1903) 0.547 (0.1714)- + - + 0.473 (0.1039) 0.469 (0.1538) 0.584 (0.2878) 0.584 (0.3031)- + - - 0.348 (0.1497) 0.414 (0.1209) 0.529 (0.2778) 0.643 (0.2735)- - + + 0.358 (0.0879) 0.330 (0.0859) 0.297 (0.1226) 0.244 (0.1279)- - + - 0.249 (0.1383) 0.248 (0.2776) 0.221 (0.3129) 0.309 (0.2498)- - - + 0.243 (0.1308) 0.236 (0.2314) 0.296 (0.1947) 0.248 (0.2256)- - - - 0.158 (0.1854) 0.198 (0.1520) 0.252 (0.1261) 0.344 (0.0989)Abbreviations: SAL, Salmonella/microsome mutagenicity assay (S); ABS, chromosome aberrations (A); SCE, sister chromatid exchange (C); MLA, mouse lym-phoma L5178Y cell mutagenicity assay (M).a Standard errors are in parenthesis.(SAL+, MLA-), note in Table 4 large standard errors of theestimates ofp(CAJ STT results), particularly for (SAL+, MLA-)under the [AC] [CM] [MS] model.Earlier findings (11-13) suggest that collapsing the four-dimensional contingency table into a lower-dimensional con-tingency table does not improve the predictivities ofcarcinogenicity in Table 4. The stepwise model improvement inTable 2 is reminiscent of stepwise regression. Model improve-ment over the complete independence model first brings in[CM], the interaction ofSCE and MLA. Then [AC], the interac-tion ofABS and SCE enters into the model. It is noticeable thatSAL is weakly linked only at the third step as [MS] enters themodel. Table 4 shows how the estimates of p(CAJSTT results)change under various depencence structures of the four STTs.dependence structures of the four STTs. Most notable are thegenerally large standard errors associated with the predictedprob-abilities of carcinogenicity. Even a database of 114 chemicals isstill relatively small for this qualitative prediction. Investigatorsinterested in applying this methodology to analysis oftheir owndata, proprietary or otherwise, need to appreciate the relationshipbetween precision ofthe prediction and the size ofthe availabledatabase. The standard errors ofthe estimates serve this purpose.Finally, why should biological end points as diverse as the fourSTTs considered here show dependence? Is there a commonprecursor, such as genomic fluidity? Irrespective ofthe explana-tion for the dependence, Kuroki and Matsushima (17) were cor-rect when they wrote,Although there have been a number of studies on the correlationof results of short-term tests with carcinogenicity, not much attentionhas been paid to the correlation between results of short-term tests. However, this is important in evaluating short-term testsand determining complementary assays that in combination may in-crease predictive values. Such correlations may suggest cellular andmolecular mechanisms by which a given chemical causes cancer.R=ERCES1. Heinze, J. E., and Pbulsen, N. K. Theoptimal designofbatteries ofshort-term tests for detecting carcinogens. Mutat. Res. 117: 259-269 (1983).2. Rosenkranz, H. S., Klopman, G., Chankong, V., Pet-Edwards, J., andHaimes, Y. Y. Prediction ofenvironmental carcinogens: a strategy for themid-1980s. Environ. Mutagen. 6: 231-258 (1984).3. Chankong, V., Haimes, Y. Y., Rosenkranz, H. S., and Pet-Edwards, J. Thecarcinogenicity prediction and battery selection (CPBS) method: a Baye-sian approach. Mutat. Res. 153: 135-166 (1985).4. Pet-Edwards, J., Chankong, V., Rosenkranz, H. S., and Haimes, Y. Y. Ap-plication of the carcinogenicity prediction and battery selection (CPBS)method to the Gene Tox data base. Mutat. Res. 153: 187-200 (1985).5. Ennever, F. K., and Rosenkranz, H. S. Short-term test results for NTP non-carcinogens: an alternate, more precise battery. Environ. Mutagen. 8:849-865 (1986).6. Ennever, F. K., and Rosenkranz, H. S. Application ofthe carcinogenicityprediction and battery selection method to recent National Toxicology Pro-gram short-term test data. Environ. Mol. Mutagen. 13: 332-338 (1989).7. Denniston, C Screening program theory: decision functions and protocols.Environ. Mutagen. 7: 53-72 (1985).8. Lave, L. B., and Omenn, G. S. Cost effectiveness of short-term tests for car-cinogenicity. Nature 324: 29-34 (1986).9. Ennever, F. K., and Rosenkranz, H. S. Prediction of carcinogenic poten-cy by short-term genotoxicity tests. Mutagenesis 2: 39-44 (1987).10. Purchase, I. F. H., Longstaff, E., Ashby J., Styles, J. A., Anderson, D.,Lefevre, P. A., and Westwood, F. R. An evaluation of6 short-term tests fordetecting organic chemical carcinogens. Br. J. Cancer. 37: 873-959 (1978).11. Tennant, R. W., Margolin, B. H., Shelby, M. D., Zeiger, E., Haseman, J.K., Spalding, J., Caspary, W., Resnick, M., Stasiewicz, S., Anderson, B.,and Minor, R. Prediction of chemical carcinogenicity in rodents from invitro genetic toxicity assays. Science 236: 933-941 (1987).12. Zeiger, E., Haseman, J. K., Shelby, M. D., Margolin, B. H., and Tennant,R. W. Evaluation offour in vitro genetic toxicity tests for predicting rodentcarcinogenicity: confirnationof earlier results with 41 additional chemicals.Environ. Mol. Mutagen. 16:(suppl. 18): 1-14 (1990).13. Haseman, J. K., Zeiger, E., Shelby, M. D., Margolin, B. H. and Tennant,R. W. Predicting rodent carcinogenicity from four in vitro genetic toxici-ty assays: anevaluation of 114chemicals studied by the National ToxicologyProgram. J. Am. Stat. Assoc. 85: 964-971 (1990)14. Fienberg, S. E., The Analysis ofCross-Classified Categorical Data. MITPress, Cambridge, MA, 1980.15. Fingleton, B. Models ofCategory Counts. Cambridge University Press,Cambridge, 1984.16. SAS Institute Inc. SAS Users Guide: Statistics, Version 5 ed. Cary, NC,1985.17. Kuroki, T., and Matsushima, T. Performance ofshort-term tests for detec-tion ofhuman carcinogens. Mutagenesis 2: 33-37 (1987).

Predicting carcinogenicity by using batteries of dependent short-term tests

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Predicting carcinogenicity by using batteries of dependent short-term tests.

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