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肿瘤细胞迁移建模:从微观模型到宏观模型。

Modeling tumor cell migration: From microscopic to macroscopic models.

作者信息

Deroulers Christophe, Aubert Marine, Badoual Mathilde, Grammaticos Basil

机构信息

IMNC, Universités Paris VII-Paris XI-CNRS, UMR 8165, Bâtiment 104, 91406 Orsay Cedex, France.

出版信息

Phys Rev E Stat Nonlin Soft Matter Phys. 2009 Mar;79(3 Pt 1):031917. doi: 10.1103/PhysRevE.79.031917. Epub 2009 Mar 25.

Abstract

It has been shown experimentally that contact interactions may influence the migration of cancer cells. Previous works have modelized this thanks to stochastic, discrete models (cellular automata) at the cell level. However, for the study of the growth of real-size tumors with several million cells, it is best to use a macroscopic model having the form of a partial differential equation (PDE) for the density of cells. The difficulty is to predict the effect, at the macroscopic scale, of contact interactions that take place at the microscopic scale. To address this, we use a multiscale approach: starting from a very simple, yet experimentally validated, microscopic model of migration with contact interactions, we derive a macroscopic model. We show that a diffusion equation arises, as is often postulated in the field of glioma modeling, but it is nonlinear because of the interactions. We give the explicit dependence of diffusivity on the cell density and on a parameter governing cell-cell interactions. We discuss in detail the conditions of validity of the approximations used in the derivation, and we compare analytic results from our PDE to numerical simulations and to some in vitro experiments. We notice that the family of microscopic models we started from includes as special cases some kinetically constrained models that were introduced for the study of the physics of glasses, supercooled liquids, and jamming systems.

摘要

实验表明,接触相互作用可能会影响癌细胞的迁移。先前的研究通过细胞水平的随机离散模型(细胞自动机)对此进行了建模。然而,对于研究具有数百万个细胞的实际大小肿瘤的生长情况,最好使用一个以细胞密度的偏微分方程(PDE)形式的宏观模型。困难在于预测微观尺度上发生的接触相互作用在宏观尺度上的影响。为了解决这个问题,我们采用多尺度方法:从一个非常简单但经过实验验证的具有接触相互作用的迁移微观模型出发,推导出一个宏观模型。我们表明出现了一个扩散方程,这在胶质瘤建模领域中经常被假设,但由于相互作用它是非线性的。我们给出了扩散率对细胞密度和控制细胞 - 细胞相互作用的参数的明确依赖关系。我们详细讨论了推导过程中所用近似的有效性条件,并将我们的偏微分方程的解析结果与数值模拟以及一些体外实验进行了比较。我们注意到我们所采用的微观模型族作为特殊情况包括一些为研究玻璃、过冷液体和堵塞系统的物理性质而引入的动力学受限模型。

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