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多细胞肿瘤球体中细胞的迁移。

The migration of cells in multicell tumor spheroids.

作者信息

Pettet G J, Please C P, Tindall M J, McElwain D L

机构信息

CiSSaIM, School of Mathematical Sciences, Queensland University of Technology, GPO Box 2434, Brisbane, QLD 4001, Australia.

出版信息

Bull Math Biol. 2001 Mar;63(2):231-57. doi: 10.1006/bulm.2000.0217.

DOI:10.1006/bulm.2000.0217
PMID:11276525
Abstract

A mathematical model is proposed to explain the observed internalization of microspheres and 3H-thymidine labelled cells in steady-state multicellular spheroids. The model uses the conventional ideas of nutrient diffusion and consumption by the cells. In addition, a very simple model of the progress of the cells through the cell cycle is considered. Cells are divided into two classes, those proliferating (being in G1, S, G2 or M phases) and those that are quiescent (being in G0). Furthermore, the two categories are presumed to have different chemotactic responses to the nutrient gradient. The model accounts for the spatial and temporal variations in the cell categories together with mitosis, conversion between categories and cell death. Numerical solutions demonstrate that the model predicts the behavior similar to existing models but has some novel effects. It allows for spheroids to approach a steady-state size in a non-monotonic manner, it predicts self-sorting of the cell classes to produce a thin layer of rapidly proliferating cells near the outer surface and significant numbers of cells within the spheroid stalled in a proliferating state. The model predicts that overall tumor growth is not only determined by proliferation rates but also by the ability of cells to convert readily between the classes. Moreover, the steady-state structure of the spheroid indicates that if the outer layers are removed then the tumor grows quickly by recruiting cells stalled in a proliferating state. Questions are raised about the chemotactic response of cells in differing phases and to the dependency of cell cycle rates to nutrient levels.

摘要

提出了一个数学模型来解释在稳态多细胞球体中观察到的微球和3H-胸腺嘧啶核苷标记细胞的内化现象。该模型采用了细胞营养物质扩散和消耗的传统概念。此外,还考虑了一个非常简单的细胞通过细胞周期进展的模型。细胞分为两类,一类是增殖细胞(处于G1、S、G2或M期),另一类是静止细胞(处于G0期)。此外,假定这两类细胞对营养梯度具有不同的趋化反应。该模型考虑了细胞类别随时间和空间的变化以及有丝分裂、类别间的转换和细胞死亡。数值解表明,该模型预测的行为与现有模型相似,但有一些新颖的效应。它允许球体以非单调的方式接近稳态大小,它预测细胞类别会自我分类,在外表面附近产生一层快速增殖的细胞薄层,并且球体内有大量细胞停滞在增殖状态。该模型预测,肿瘤的总体生长不仅取决于增殖率,还取决于细胞在不同类别之间轻松转换的能力。此外,球体的稳态结构表明,如果去除外层,肿瘤会通过募集停滞在增殖状态的细胞而快速生长。文中还提出了关于不同阶段细胞的趋化反应以及细胞周期速率对营养水平的依赖性的问题。

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