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首页> 外文期刊>Cytometry, Part A: the journal of the International Society for Analytical Cytology >Individual cell-based models of the spatial-temporal organization of multicellular systems - Achievements and limitations
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Individual cell-based models of the spatial-temporal organization of multicellular systems - Achievements and limitations

机译:多细胞系统的时空组织的基于单个细胞的模型-成就和局限性

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Computational approaches of multicellular assemblies have reached a stage where they may contribute to unveil the processes that underlie the organization of tissues and multicellular aggregates. In this article, we briefly review and present some new results on a number of 3D lattice free individual cell-based mathematical models of epithelial cell populations. The models we consider here are parameterized by bio-physical and cell-biological quantities on the level of an individual cell. Eventually, they aim at predicting the dynamics of the biological processes on the tissue level. We focus on a number of systems, the growth of cell populations in vitro, and the spatial-temporal organization of regenerative tissues. For selected examples we compare different model approaches and show that the qualitative results are robust with respect to many model details. Hence, for the qualitative features and largely for the quantitative features many model details do not matter as long as characteristic biological features and mechanisms are correctly represented. For a quantitative prediction, the control of the bio-physical and cell-biological parameters on the molecular scale has to be known. At this point, slide-based cytometry may contribute. It permits to track the fate of cells and other tissue subunits in time and validated the organization processes predicted by the mathematical models. (c) 2006 international Society for Analytical Cytology.
机译:多细胞集合体的计算方法已经达到了一个阶段,它们可能有助于揭示构成组织和多细胞聚集体基础的过程。在本文中,我们简要回顾并提出了一些关于上皮细胞群体的无3D晶格独立细胞模型的一些新结果。我们在这里考虑的模型是由单个细胞水平上的生物物理量和细胞生物学量参数化的。最终,它们旨在预测组织水平上生物过程的动力学。我们专注于许多系统,体外细胞群的生长以及再生组织的时空组织。对于选定的示例,我们比较了不同的模型方法,并表明定性结果在许多模型细节方面均很可靠。因此,对于定性特征和很大程度上对于定量特征,只要正确地表征特征生物学特征和机理,许多模型细节就无关紧要。为了进行定量预测,必须知道在分子尺度上对生物物理和细胞生物学参数的控制。在这一点上,基于玻片的细胞计数法可能起作用。它允许及时跟踪细胞和其他组织亚基的命运,并验证数学模型预测的组织过程。 (c)2006年国际分析细胞学学会。

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