nach oben

Erschienen in:

2020 | OriginalPaper | Buchkapitel

Multistage Carcinogenesis: A Unified Framework for Cancer Data Analysis

verfasst von : Suresh Moolgavkar, Georg Luebeck

Erschienen in: Statistical Modeling for Biological Systems

Verlag: Springer International Publishing

Einloggen

Aktivieren Sie unsere intelligente Suche, um passende Fachinhalte oder Patente zu finden.

search-config

KI-gestützte Suche

Aus

Abstract

Traditional approaches to the analysis of epidemiologic data are focused on estimation of the relative risk and are based on the proportional hazards model. Proportionality of hazards in epidemiologic data is a strong assumption that is often violated but seldom checked. Risk often depends on detailed patterns of exposure to environmental agents, but detailed exposure histories are difficult to incorporate in the traditional approaches to analyses of epidemiologic data. For epidemiologic data on cancer, an alternative approach to analysis can be based on ideas of multistage carcinogenesis. The process of carcinogenesis is characterized by mutation accumulation and clonal expansion of partially altered cells on the pathway to cancer. Although this paradigm is now firmly established, most epidemiologic studies of cancer incorporate ideas of multistage carcinogenesis neither in their design nor in their analyses. In this paper we will briefly discuss stochastic multistage models of carcinogenesis and the construction of the appropriate likelihoods for analyses of epidemiologic data using these models. Statistical analyses based on multistage models can quite explicitly incorporate detailed exposure histories in the construction of the likelihood. We will give examples to show that using ideas of multistage carcinogenesis can help reconcile seemingly contradictory findings, and yield insights into epidemiologic studies of cancer that would be difficult or impossible to get from conventional methods. Finally, multistage cancer models provide a unified framework for analyses of data from diverse sources.

Sie haben noch keine Lizenz? Dann Informieren Sie sich jetzt über unsere Produkte:

Springer Professional "Wirtschaft+Technik"

Online-Abonnement

Mit Springer Professional "Wirtschaft+Technik" erhalten Sie Zugriff auf:

über 102.000 Bücher
über 537 Zeitschriften

aus folgenden Fachgebieten:

Automobil + Motoren
Bauwesen + Immobilien
Business IT + Informatik
Elektrotechnik + Elektronik
Energie + Nachhaltigkeit
Finance + Banking
Management + Führung
Marketing + Vertrieb
Maschinenbau + Werkstoffe
Versicherung + Risiko

Jetzt Wissensvorsprung sichern!

Jetzt informieren

Springer Professional "Technik"

Online-Abonnement

Mit Springer Professional "Technik" erhalten Sie Zugriff auf:

über 67.000 Bücher
über 390 Zeitschriften

aus folgenden Fachgebieten:

Automobil + Motoren
Bauwesen + Immobilien
Business IT + Informatik
Elektrotechnik + Elektronik
Energie + Nachhaltigkeit
Maschinenbau + Werkstoffe

Jetzt Wissensvorsprung sichern!

Jetzt informieren

Springer Professional "Wirtschaft"

Online-Abonnement

Mit Springer Professional "Wirtschaft" erhalten Sie Zugriff auf:

über 67.000 Bücher
über 340 Zeitschriften

aus folgenden Fachgebieten:

Bauwesen + Immobilien
Business IT + Informatik
Finance + Banking
Management + Führung
Marketing + Vertrieb
Versicherung + Risiko

Jetzt Wissensvorsprung sichern!

Jetzt informieren

Vorheriges Kapitel Applications of Sequential Methods in Multiple Hypothesis Testing

Nächstes Kapitel A Machine-Learning Algorithm for Estimating and Ranking the Impact of Environmental Risk Factors in Exploratory Epidemiological Studies

Parameters would be expected to return to background levels with exposure to agents, such as benzene, that are rapidly cleared from the body. Other agents, such as amphibole asbestos, accumulate in tissues, and after exposure to such agents stops, the parameters of the model could remain altered for a long period of time and would be expected to return to background levels only slowly as the agent is excreted from tissues.

Armitage, P., & Doll, R. (1954). The age distribution of cancer and a multi-stage theory of carcinogenesis. British Journal of Cancer, 8, 1–12.CrossRef

Berenblum, I., & Shubik, P. (1947). A new, quantitative approach to the study of the stages of chemical carcinogenesis in the mouse’s skin. British Journal of Cancer, 1, 383–391.CrossRef

Berman, D. W., & Crump, K. S. (2008). Update of potency factors for asbestos-related lung cancer and mesothelioma. Critical Reviews in Toxicology, 38(Suppl 1), 1–47.CrossRef

Bozic, I., Antal, T., Ohtsuki, H., Carter, H., Kim, D., Chen, S., et al. (2010). Accumulation of driver and passenger mutations during tumor progression. Proceedings of the National Academy of Sciences, 107(43), 18545–18550.CrossRef

Breslow, N. (1974). Covariance analysis of censored survival data. Biometrics, 30(1), 89–99.CrossRefMathSciNet

Brouwer, A. F., Meza, R., & Eisenberg, M. C. (2017). Parameter estimation for multistage clonal expansion models from cancer incidence data: A practical identifiability analysis. PLoS Computational Biology, 13(3), e1005431–18.CrossRef

Brown, C. C., & Chu, K. C. (1983). Implications of the multistage theory of carcinogenesis applied to occupational arsenic exposure. Journal of the National Cancer Institute, 70, 455–463.

Burns, D. M., Shanks, T. G., Choi, W., Thun, M. J., Heath, C. W., & Garfinkel, L. (1997). The American Cancer Society Cancer Prevention Study I: 12-year followup of 1 million men and women. In D. M. Burns, L. Garfinkel, & J. M. Samet (Eds.) Smoking and tobacco control, monograph 8 (pp. 113–304). NIH Publ. No 97-4213.

Cole, B. F., Baron, J. A., Sandler, R. S., Haile, R. W., Ahnen, D. J., Bresalier, R. S., et al. (2007). Folic acid for prevention of colorectal adenomas. A randomized clinical trial. JAMA : The Journal of the American Medical Association, 297, 2351–2359.CrossRef

10.

Cox, D. R. (1972). Regression models and life tables (with discussion). Journal of the Royal Statistical Society, Series B: Statistical Methodology, 34, 187–220.MATH

11.

Crump, K. S., Chen, C., Fox, J. F., Van Landingham, C., & Subramaniam, R. (2008). Sensitivity analysis of biologically motivated model for formaldehyde-induced respiratory cancer in humans. The Annals of Occupational Hygiene, 52, 481–95.

12.

Crump, K. S., Subramaniam, R. P., & Landigham, C. B. (2005). A numerical solution to the nonhomogeneous two-stage MVK model of cancer. Risk Analysis, 25, 921–926.CrossRef

13.

Day, N. E., & Brown, C. C. (1980). Multistage models and the primary prevention of cancer. Journal of the National Cancer Institute, 64, 977–989.

14.

Dewanji, A., Jeon, J., Meza, R., & Luebeck, E. G. (2011). Number and size distribution of colorectal adenomas under the multistage clonal expansion model of cancer. PLoS Computational Biology, 7(10), e1002213.CrossRefMathSciNet

15.

Dewanji, A., Venzon, D. J., & Moolgavkar, S. H. (1989). A stochastic two-stage model for cancer risk assessment II: The number and size of premalignant clones. Risk Analysis, 9, 179–186.CrossRef

16.

Doll, R., & Peto, R. (1978). Cigarette smoking and bronchial carcinoma: Dose and time relationships among regular smokers and life-long non-smokers. Journal of Epidemiology and Community Health, 32, 303–313.CrossRef

17.

Efron, B., & Morris, C. (1977). Comment on A Simulation Study of Alternative to Least Squares, by H. Clark and T. Schwisow. The American Statistician, 72, 102–109.

18.

Hanin, L. G., & Yakovlev, A. Y. (1996). A nonidentifiability aspect of the two-stage model of carcinogenesis. Risk Analysis, 16, 711–715.CrossRef

19.

Hazelton, W. D., Clements, M. S., & Moolgavkar, S. H. (2005). Multistage carcinogenesis and lung cancer mortality in three cohorts. Cancer Epidemiology, Biomarkers & Prevention, 14, 1171–1181.CrossRef

20.

Hazelton, W. D., Luebeck, E. G., Heidenreich, W. F., & Moolgavkar, S. H., (2001). Analysis of a historical cohort of Chinese tin miners with arsenic, radon, cigarette smoke, and pipe smoke exposures using the biologically based two-stage clonal expansion model. Radiation Research, 156(1), 78–94.CrossRef

21.

Heidenreich, W. (1996). On the parameters of the clonal expansion model. Radiation and Environmental Biophysics, 35, 127–129.CrossRef

22.

Heidenreich, W., Luebeck, E. G., & Moolgavkar, S. H. (1997). Some properties of the hazard function of the two-mutation clonal expansion model. Risk Analysis, 17, 391–399.CrossRef

23.

Heidenreich, W., Wellmann, J., Jacob, P., & Wichmann, H. E. (2002). Mechanistic modelling in large case-control studies of lung cancer risk from smoking. Statistics in Medicine, 21, 3055–3070.CrossRef

24.

Hethcote, H. W., & Knudson, A. G. (1978). Model for the incidence of embryonal cancer: application to retinoblastoma. Proceedings of the National Academy of Sciences of the United States of America, 75, 2453–2457.

25.

Holford, T. R. (1991). Understanding the effects of age, period and cohort on incidence and mortality rates. Annual Review of Public Health, 12, 425–457.CrossRef

26.

Holford, T. R., Zhang, Z., McKay, L. A. (1994). Estimating age, period and cohort effects using the multistage model for cancer. Statistics in Medicine, 13, 23–41.CrossRef

27.

Howard, S. (1972). Contribution to the discussion of a paper by DR Cox: Regression models and life-tables. Journal of the Royal Statistical Society. Series B, 34, 210–211.

28.

Jeon, J., Luebeck, E. G., & Moolgavkar, S. H. (2006). Age effects and temporal trends in adenocarcinoma of esophagus and gastric cardia. Cancer Causes Control, 17, 971–981.CrossRef

29.

Jeon, J., Meza, R., Hazelton, W. D., Renehan, A. G., & Luebeck, E. G. (2015). Incremental benefits of screening colonoscopy over sigmoidoscopy in average-risk populations: a model-driven analysis. Cancer Causes & Control, 26(6), 859–870.CrossRef

30.

Jeon, J., Meza, R., Moolgavkar, S. H., & Luebeck, E. G. (2008). The evaluation of cancer screening strategies using multistage carcinogenesis models. Mathematical Biosciences, 213, 56–70.CrossRefMathSciNetMATH

31.

Jones, S., Chen, W., Parmigiani, G., Diehl, F., Beerenwinkel, N., Antal, T., et al. (2008). Comparative lesion sequencing provides insights into tumor evolution. Proceedings of the National Academy of Sciences, 105(11), 4283–4288.CrossRef

32.

Knudson, A. G. (2001). Two genetic hits (more or less) to cancer. Nature Reviews Cancer, 1(2), 157.CrossRef

33.

Knudson, A. G., Hethcote, H. W., & Brown, B. W. (1975). Mutation and childhood cancer: A probabilistic model for the incidence of retinoblastoma. Proceedings of the National Academy of Sciences USA, 72, 5116–5120.

34.

Langholz, B. (2010). Case-control studies = odds ratios. Blame the retrospective model. Epidemiology, 21, 10–12.CrossRef

35.

Little, M. P. (1995). Are two mutations sufficient to cause cancer? Some generalizations of the two mutation model of carcinogenesis of Moolgavkar, Venzon and Knudson, and of the multistage model of Armitage and Doll. Biometrics, 51, 1278–1291.CrossRefMATH

36.

Little, M. P. (2010). Cancer models, genomic instability and somatic cellular Darwinian evolution. Biology Direct, 5, 19.CrossRef

37.

Little, M. P., Heidenreich, W. F., & Li, G. (2009). Parameter identifiability and redundancy in a general class of stochastic carcinogenesis models. PLoS One, 4(12), e8520.CrossRef

38.

Luebeck, E. G., Buchmann, A., Stinchcombe, S., Moolgavkar, S. H., & Schwarz, M. (2000). Effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) on initiation and promotion of GSTP-positive foci in rat liver: A quantitative analysis of experimental data using a stochastic model. Toxicology and Applied Pharmacology, 167, 63–73.CrossRef

39.

Luebeck, E. G., Curtis, S. B., Cross, F. T., & Moolgavkar, S. H. (1996). Two-stage model of radon-induced malignant lung tumors in rats: effects of cell killing. Radiation Research, 145(2), 163–173.CrossRef

40.

Luebeck, E. G., Curtius, K., Jeon, J., & Hazelton, W. D. (2013). Impact of tumor progression on cancer incidence curves. Cancer Research, 73(3), 2198.CrossRef

41.

Luebeck, E. G., & Moolgavkar, S. H. (2002). Multistage carcinogenesis and the incidence of colorectal cancer. Proceedings of the National Academy of Sciences of the United States of America, 99, 15095–15100.

42.

Luebeck, E. G., Moolgavkar, S. H., Buchmann, A., & Schwarz, M. (1991). Effects of polychlorinated biphenyls in rat liver: Quantitative analysis of enzyme-altered foci. Toxicology and Applied Pharmacology, 111(3), 469–484.CrossRef

43.

Luebeck, E. G., Moolgavkar, S. H., Liu, A., & Ulrich, N. (2008). Does folic acid supplementation prevent or promote colon cancer? Results from model-based predictions. Cancer Epidemiology, Biomarkers & Prevention, 17, 1360–1367.CrossRef

44.

Mason, J. B., Dickstein, A., Jacques, P. F., Haggarty, P., Selhub, J., Dallal, G. et al. (2007). A temporal association between folic acid fortification and an increase in colorectal cancer rates may be illuminating important biological principles: a hypothesis. Cancer Epidemiology, Biomarkers & Prevention, 16, 1325–1329.CrossRef

45.

Meza, R., Hazelton, W. D., Colditz, G. A., & Moolgavkar, S. H. (2008a). Analysis of lung cancer incidence in the nurses’ health and the health professionals’ follow-up studies using a multistage carcinogenesis model. Cancer Causes Control, 19, 317–328.CrossRef

46.

Meza, R., Jeon, J., Moolgavkar, S. H., & Luebeck, E. G. (2008b). The age-specific incidence of cancer: phases, transitions and biological implications. Proceedings of the National Academy of Sciences of the United States of America, 105, 16284–16289.

47.

Moolgavkar, S. H. (1995). When and how to combine results from multiple epidemiological studies in risk assessment. In J. Graham (ed.) The proper role of epidemiology in regulatory risk assessment (pp. 77–90). New York: Elsevier.

48.

Moolgavkar, S. H., Chang, E. T., Watson, H. N., & Lau, E. C. (2018). An assessment of the cox proportional hazards regression model for epidemiologic studies. Risk Analysis, 38(4), 777–794.CrossRef

49.

Moolgavkar, S. H., Day, N. E., & Stevens, R. G. (1980). Two-stage model for carcinogenesis: Epidemiology of breast cancer in females. Journal of the National Cancer Institute, 65, 559–569.

50.

Moolgavkar, S. H., Krewski, D., & Schwarz, M. (1999). Mechanisms of carcinogenesis and biologically-based models for quantitative estimation and prediction of cancer risk. In S. H. Moolgavkar, D. Krewski, L. Zeise, E. Cardis, & H. Moller (Eds.) Quantitative estimation and prediction of cancer risk (pp. 179–238). Lyon: IARC Scientific Publications.

51.

Moolgavkar, S. H., & Luebeck, G. (1990). Two-event model for carcinogenesis: Biological, mathematical and statistical considerations. Risk Analysis, 10, 323–341.CrossRef

52.

Moolgavkar, S. H., & Luebeck, E. G. (1992). Multistage carcinogenesis: A population-based model for colon cancer. Journal of the National Cancer Institute, 84, 610–618.CrossRef

53.

Moolgavkar, S. H., Luebeck, E. G., de Gunst, M., Port, R. E., & Schwarz, M. (1990). Quantitative analysis of enzyme altered foci in rat hepatocarcinogenesis experiments. Carcinogenesis, 11, 1271–1278.CrossRef

54.

Moolgavkar, S. H., Luebeck, E. G., Turim, J., & Brown, R. C. (2000). Lung cancer risk associated with exposure to man-made fibers. Drug and Chemical Toxicology, 23(1), 223–242.CrossRef

55.

Moolgavkar, S. H., Meza, R., & Turim, J. (2009). Pleural and peritoneal mesotheliomas in SEER: Age effects and temporal trends, 1973–2005. Cancer Causes & Control, 20(6), 935–944.CrossRef

56.

Moolgavkar, S. H., Turim, J., Alexander, D. D., Lau, E. C., & Cushing, C. A. (2010). Potency factors for risk assessment at Libby, Montana. Risk Analysis, 30, 1240–1248.CrossRef

57.

Moolgavkar, S. H., & Venzon, D. J. (1979). Two-event model for carcinogenesis: Incidence curves for childhood and adult tumors. Mathematical Biosciences, 47, 55–77.CrossRefMATH

58.

Peto, J. (2012). That the effects of smoking should be measured in pack-years: Misconceptions. British Journal of Cancer, 107(3), 406–407.CrossRef

59.

Peto, J., Seidman, H., & Selikoff, I. J. (1982). Mesothelioma mortality in asbestos workers: Implications for models of carcinogenesis and risk assessment. British Journal of Cancer, 45, 124–135.CrossRef

60.

Peto, R. (1972). Contribution to discussion paper by D. R. Cox: Regression models and life-tables. Journal of the Royal Statistical Society, Serial B, 34, 205–207.MathSciNet

61.

Poole, C. (2010). On the origin of risk relativism. Epidemiology, 21, 3–9.CrossRef

62.

Prentice, R. L., & Breslow N. E. (1978). Retrospective studies and failure time models. Biometrika, 65(1), 153–158.CrossRefMATH

63.

Prentice, R. L., & Kalbfleisch, J. D. (1979). Hazard rate models with covariates. Biometrics, 35(1), 25–39.CrossRefMathSciNetMATH

64.

Rachet, B., Siemiatycki, J., Abrahamowicz, M., & Leffondre, K. (2004). A flexible modeling approach to estimating the component effects of smoking behavior on lung cancer. Journal of Clinical Epidemiology, 57, 1076–1085.CrossRef

65.

Richardson, D. B. (2008). Temporal variation in the association between benzene and leukemia mortality. Environmental Health Perspectives, 116, 370–374.CrossRef

66.

Richardson, D. B. (2009). Multistage modeling of leukemia in benzene workers: a simple approach to fitting the 2-stage clonal expansion model. American Journal of Epidemiology, 169, 78–85.CrossRef

67.

Sullivan, P. A. (2007). Vermiculite, respiratory disease, and asbestos exposure in Libby, Montana. Update of a cohort mortality study. Environmental Health Perspectives, 115, 579–585.CrossRef

68.

Surveillance, Epidemiology, and End Results (SEER) Program Research Data. (1973–2015). National Cancer Institute, DCCPS, Surveillance Research Program, released April 2018, based on the November 2017 submission. www.seer.cancer.gov.

69.

Thomas, D. C. (1983). Statistical methods for analyzing effects of temporal patterns of exposure on cancer risks. Scandinavian Journal of Work, Environment & Health, 9, 353–366.CrossRef

70.

Thomas, D. C. (1988). Models for exposure-time-response relationships with applications to cancer epidemiology. Annual Review of Public Health, 9, 451–482.CrossRef

71.

Thomas, D. C. (2014). Invited commentary: Is it time to retire the pack-years variable? Maybe not! American Journal of Epidemiology, 179(3), 299–302.CrossRef

72.

Tomasetti, C., Li, L., & Vogelstein, B. (2017). Stem cell divisions, somatic mutations, cancer etiology, and cancer prevention. Science, 355(6331), 1330–1334.CrossRef

73.

Tomasetti, C., Marchionni, L., Nowak, M. A., Parmigiani, G., & Vogelstein, B. (2015). Only three driver gene mutations are required for the development of lung and colorectal cancers. Proceedings of the National Academy of Sciences, 112(1), 118–123.CrossRef

74.

Tomasetti, C., & Vogelstein, B. (2015). Variation in cancer risk among tissues can be explained by the number of stem cell divisions. Science, 347(6217), 78–81.CrossRef

75.

Triebig, G. (2010). Implications of latency period between benzene exposure and development of leukemia – A synopsis of literature. Chemico-Biological Interactions, 184, 26–29.CrossRef

76.

Vogelstein, B., & Kinzler, K. W. (2015). The path to cancer – Three strikes and you’re out. The New England Journal of Medicine, 373(20), 1895–1898.CrossRef

77.

Whittemore, A. S. (1977). The age distribution of human cancer for carcinogenic exposures of varying intensity. American Journal of Epidemiology, 109, 709–718.

Titel: Multistage Carcinogenesis: A Unified Framework for Cancer Data Analysis
verfasst von: Suresh Moolgavkar
Georg Luebeck
Verlag: Springer International Publishing
Buch: Statistical Modeling for Biological Systems
Print ISBN: 978-3-030-34674-4

Electronic ISBN: 978-3-030-34675-1

Copyright-Jahr: 2020
DOI: https://doi.org/10.1007/978-3-030-34675-1_7

Springer Professional

Abstract

Bitte loggen Sie sich ein, um Zugang zu Ihrer Lizenz zu erhalten.

Sie haben noch keine Lizenz? Dann Informieren Sie sich jetzt über unsere Produkte:

Springer Professional "Wirtschaft+Technik"

Springer Professional "Technik"

Springer Professional "Wirtschaft"

Premium Partner