A Multicompartment Mathematical Model of Cancer Stem Cell-Driven Tumor Growth Dynamics

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作者
Suzanne L. Weekes
Brian Barker
Sarah Bober
Karina Cisneros
Justina Cline
Amanda Thompson
Lynn Hlatky
Philip Hahnfeldt
Heiko Enderling
机构
[1] Worcester Polytechnic Institute,Department of Mathematical Sciences
[2] University of Rochester,Department of Mathematics
[3] Dominican University,Department of Mathematics
[4] Coe College,Department of Mathematics and Computer Science
[5] University of North Carolina at Chapel Hill,Department of Mathematics
[6] Tufts University School of Medicine,Center of Cancer Systems Biology, GeneSys Research Institute
[7] H. Lee Moffitt Cancer Center & Research Institute,Department of Integrated Mathematical Oncology
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Cancer stem cells; Mathematical model; Cancer progression; Age structure; Compartment model;
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摘要
Tumors are appreciated to be an intrinsically heterogeneous population of cells with varying proliferation capacities and tumorigenic potentials. As a central tenet of the so-called cancer stem cell hypothesis, most cancer cells have only a limited lifespan, and thus cannot initiate or reinitiate tumors. Longevity and clonogenicity are properties unique to the subpopulation of cancer stem cells. To understand the implications of the population structure suggested by this hypothesis—a hierarchy consisting of cancer stem cells and progeny non-stem cancer cells which experience a reduction in their remaining proliferation capacity per division—we set out to develop a mathematical model for the development of the aggregate population. We show that overall tumor progression rate during the exponential growth phase is identical to the growth rate of the cancer stem cell compartment. Tumors with identical stem cell proportions, however, can have different growth rates, dependent on the proliferation kinetics of all participating cell populations. Analysis of the model revealed that the proliferation potential of non-stem cancer cells is likely to be small to reproduce biologic observations. Furthermore, a single compartment of non-stem cancer cell population may adequately represent population growth dynamics only when the compartment proliferation rate is scaled with the generational hierarchy depth.
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页码:1762 / 1782
页数:20
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