A Microenvironment Based Model of Antimitotic Therapy of Gompertzian Tumor Growth |
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| Authors: | Frank Kozusko Michele Bourdeau Zeljko Bajzer David Dingli |
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| Institution: | (1) Department of Mathematics, Hampton University, Hampton, VA 23668, USA;(2) Lehman Brothers, New York, NY 10019, USA;(3) Biomathematics Resource, Mayo Clinic College of Medicine, Rochester, MN 55905, USA;(4) Division of Hematology, Mayo Clinic College of Medicine, Rochester, MN 55905, USA;(5) Program for Evolutionary Dynamics, Harvard University, One Brattle Square, Ste 6, Cambridge, MA 02138, USA |
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| Abstract: | A model of tumor growth, based on two-compartment cell population dynamics, and an overall Gompertzian growth has been previously
developed. The main feature of the model is an inter-compartmental transfer function that describes the net exchange between
proliferating (P) and quiescent (Q) cells and yields Gompertzian growth for tumor cell population N = P + Q. Model parameters provide for cell reproduction and cell death. This model is further developed here and modified to simulate
antimitotic therapy. Therapy decreases the reproduction-rate constant and increases the death-rate constant of proliferating
cells with no direct effect on quiescent cells. The model results in a system of two ODE equations (in N and P/N) that has an analytical solution. Net tumor growth depends on support from the microenvironment. Indirectly, this is manifested
in the transfer function, which depends on the proliferation ratio, P/N. Antimitotic therapy will change P/N, and the tumor responds by slowing the transfer rate from P to Q. While the cellular effects of therapy are modeled as dependent only on antimitotic activity of the drug, the tumor response
also depends on the tumor age and any previous therapies—after therapy, it is not the same tumor. The strength of therapy is simulated by the parameter λ, which is the ratio of therapy induced net proliferation rate constant versus the original. A pharmacodynamic factor inversely
proportional to tumor size is implemented. Various chemotherapy regimens are simulated and the outcomes of therapy administered
at different time points in the life history of the tumor are explored. Our analysis shows: (1) for a constant total dose
administered, a decreasing dose schedule is marginally superior to an increasing or constant scheme, with more pronounced
benefit for faster growing tumors, (2) the minimum dose to stop tumor growth is age dependent, and (3) a dose-dense schedule
is favored. Faster growing tumors respond better to dose density. |
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| Keywords: | Gompertz Chemotherapy Cell kinetics Proliferation Tumor |
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