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A model for cell migration in non-isotropic fibrin networks with an application to pancreatic tumor islets

机译:非各向同性纤维蛋白网络中细胞迁移的模型及其在胰腺肿瘤胰岛中的应用

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摘要

Cell migration, known as an orchestrated movement of cells, is crucially important for wound healing, tumor growth, immune response as well as other biomedical processes. This paper presents a cell-based model to describe cell migration in non-isotropic fibrin networks around pancreatic tumor islets. This migration is determined by the mechanical strain energy density as well as cytokines-driven chemotaxis. Cell displacement is modeled by solving a large system of ordinary stochastic differential equations where the stochastic parts result from random walk. The stochastic differential equations are solved by the use of the classical Euler–Maruyama method. In this paper, the influence of anisotropic stromal extracellular matrix in pancreatic tumor islets on T-lymphocytes migration in different immune systems is investigated. As a result, tumor peripheral stromal extracellular matrix impedes the immune response of T-lymphocytes through changing direction of their migration.Electronic supplementary materialThe online version of this article (doi:10.1007/s10237-017-0966-7) contains supplementary material, which is available to authorized users.
机译:细胞迁移,被称为细胞的协调运动,对于伤口愈合,肿瘤生长,免疫反应以及其他生物医学过程至关重要。本文提出了一个基于细胞的模型来描述胰腺肿瘤胰岛周围非各向同性纤维蛋白网络中的细胞迁移。这种迁移取决于机械应变能密度以及细胞因子驱动的趋化性。通过求解一个大型的普通随机微分方程组对单元位移进行建模,其中随机部分是随机游动产生的。随机微分方程通过经典的Euler-Maruyama方法求解。本文研究了胰腺肿瘤胰岛中各向异性基质细胞外基质对不同免疫系统中T淋巴细胞迁移的影响。结果,肿瘤外周基质细胞外基质通过改变其迁移方向而阻碍了T淋巴细胞的免疫反应。电子补充材料本文的在线版本(doi:10.1007 / s10237-017-0966-7)包含补充材料,其中适用于授权用户。

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