Literature DB >> 23054397

Impact of tumor progression on cancer incidence curves.

E Georg Luebeck1, Kit Curtius, Jihyoun Jeon, William D Hazelton.   

Abstract

Cancer arises through a multistage process, but it is not fully clear how this process influences the age-specific incidence curve. Studies of colorectal and pancreatic cancer using the multistage clonal expansion (MSCE) model have identified two phases of the incidence curves. One phase is linear, beginning about age of 60 years, suggesting that at least two rare rate-limiting mutations occur before clonal expansion of premalignant cells. A second phase is exponential, seen in early-onset cancers occurring before the age of 60 years that are associated with premalignant clonal expansion. Here, we extend the MSCE model to include clonal expansion of malignant cells, an advance that permits study of the effects of tumor growth and extinction on the incidence of colorectal, gastric, pancreatic, and esophageal adenocarcinomas in the digestive tract. After adjusting the age-specific incidence for birth-cohort and calendar-year trends, we found that initiating mutations and premalignant cell kinetics can explain the primary features of the incidence curve. However, we also found that the incidence data of these cancers harbored information on the kinetics of malignant clonal expansion before clinical detection, including tumor growth rates and extinction probabilities on three characteristic time scales for tumor progression. In addition, the data harbored information on the mean sojourn times for premalignant clones until occurrence of either the first malignant cell or the first persistent (surviving) malignant clone. Finally, the data also harbored information on the mean sojourn time of persistent malignant clones to the time of diagnosis. In conclusion, cancer incidence curves can harbor significant information about hidden processes of tumor initiation, premalignant clonal expansion, and malignant transformation, and even some limited information on tumor growth before clinical detection.

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Year:  2012        PMID: 23054397      PMCID: PMC3746830          DOI: 10.1158/0008-5472.CAN-12-2198

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  45 in total

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4.  Analysis of lung cancer incidence in the Nurses' Health and the Health Professionals' Follow-Up Studies using a multistage carcinogenesis model.

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  39 in total

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5.  Mechanistic study on lung cancer mortality after radon exposure in the Wismut cohort supports important role of clonal expansion in lung carcinogenesis.

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Journal:  Radiat Environ Biophys       Date:  2016-06-22       Impact factor: 1.925

6.  A novel long noncoding RNA-LOWEG is low expressed in gastric cancer and acts as a tumor suppressor by inhibiting cell invasion.

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7.  Implications of Epigenetic Drift in Colorectal Neoplasia.

Authors:  Georg E Luebeck; William D Hazelton; Kit Curtius; Sean K Maden; Ming Yu; Kelly T Carter; Wynn Burke; Paul D Lampe; Christopher I Li; Cornelia M Ulrich; Polly A Newcomb; Maria Westerhoff; Andrew M Kaz; Yanxin Luo; John M Inadomi; William M Grady
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9.  Exploring the recent trend in esophageal adenocarcinoma incidence and mortality using comparative simulation modeling.

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10.  Mathematical model of colorectal cancer initiation.

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