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细胞如何感知基底的弹性?利用细胞刚柔并济模型进行分析。

How can cells sense the elasticity of a substrate? An analysis using a cell tensegrity model.

机构信息

Institute Biomedical Technology, Ghent University, De Pintelaan 185, Block B, BE-9000 Gent, Belgium.

出版信息

Eur Cell Mater. 2011 Oct 11;22:202-13. doi: 10.22203/ecm.v022a16.

Abstract

A eukaryotic cell attaches and spreads on substrates, whether it is the extracellular matrix naturally produced by the cell itself, or artificial materials, such as tissue-engineered scaffolds. Attachment and spreading require the cell to apply forces in the nN range to the substrate via adhesion sites, and these forces are balanced by the elastic response of the substrate. This mechanical interaction is one determinant of cell morphology and, ultimately, cell phenotype. In this paper we use a finite element model of a cell, with a tensegrity structure to model the cytoskeleton of actin filaments and microtubules, to explore the way cells sense the stiffness of the substrate and thereby adapt to it. To support the computational results, an analytical 1D model is developed for comparison. We find that (i) the tensegrity hypothesis of the cytoskeleton is sufficient to explain the matrix-elasticity sensing, (ii) cell sensitivity is not constant but has a bell-shaped distribution over the physiological matrix-elasticity range, and (iii) the position of the sensitivity peak over the matrix-elasticity range depends on the cytoskeletal structure and in particular on the F-actin organisation. Our model suggests that F-actin reorganisation observed in mesenchymal stem cells (MSCs) in response to change of matrix elasticity is a structural-remodelling process that shifts the sensitivity peak towards the new value of matrix elasticity. This finding discloses a potential regulatory role of scaffold stiffness for cell differentiation.

摘要

真核细胞会附着并铺展在基质上,无论是细胞自身天然产生的细胞外基质,还是人工材料,如组织工程支架。附着和铺展需要细胞通过黏附点向基质施加 nN 范围内的力,这些力由基质的弹性响应平衡。这种机械相互作用是细胞形态和最终细胞表型的一个决定因素。在本文中,我们使用了一个具有张拉整体结构的细胞有限元模型,该模型用于模拟肌动蛋白丝和微管的细胞骨架,以探索细胞感知基质硬度并适应基质硬度的方式。为了支持计算结果,我们还开发了一个分析的 1D 模型进行比较。我们发现:(i)细胞骨架的张拉整体假说足以解释基质弹性的感知;(ii)细胞的敏感性不是恒定的,而是在生理基质弹性范围内呈钟形分布;(iii)敏感性峰值在基质弹性范围内的位置取决于细胞骨架结构,特别是 F-肌动蛋白的组织。我们的模型表明,间质干细胞(MSCs)在基质弹性变化时观察到的 F-肌动蛋白重组是一种结构重塑过程,它将敏感性峰值向新的基质弹性值移动。这一发现揭示了支架刚度对细胞分化的潜在调节作用。

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