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Cell adhesion nucleation regulated by substrate stiffness: A Monte Carlo study

机译:细胞粘附成核受基质硬度调控:蒙特卡洛研究

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Cell adhesions are modulated by the interactions between cells and their surroundings, among which substrate stiffness plays an important role in mediating cellular behaviors and functions. Little is known, however, about the inherent mechanism of how nascent adhesion nucleation, as the precursor of focal adhesions, is regulated by substrate stiffness. This paper presents a microscopic model to imitate integrin clustering kinetics, where integrin diffusion, activation on elastic substrates, receptor-ligand binding and association dynamics are fully considered. Particularly, the contribution of substrate compliance to the activation energy is analyzed, leading to a description of mechanical energy barrier for stretching a substrate-bound integrin molecule from bent to extended conformations. A series of Monte Carlo simulations for integrin clustering dynamics are performed with varied substrate Young's moduli, which demonstrates that more integrins are clustered on stiffer substrates once they begin to assemble over a rigidity threshold, indicating the responsiveness of adhesion nucleation to substrate elasticity, which is in reasonable agreement with results reported previously. Also, these simulations show that the sensitivity of integrin clustering to substrate stiffness is mediated by chemical affinity between receptor-ligand pairs and that between integrins cross-linked by adapter proteins, as well as integrin density on cell membranes. The investigation offers a fascinating insight into the inherent mechanism of mechanosensing concerning integrin-mediated cell-matrix initial adhesions.
机译:细胞粘附受到细胞与其周围环境之间相互作用的调节,其中基质刚度在介导细胞行为和功能中起重要作用。然而,关于作为基质粘连的前体的新生粘连成核如何受基材刚度调节的内在机理知之甚少。本文提出了一个模拟整合素簇动力学的微观模型,其中整合素的扩散,在弹性底物上的活化,受体-配体的结合和缔合动力学都得到了充分考虑。特别地,分析了底物顺应性对活化能的贡献,从而导致了对用于将底物结合的整联蛋白分子从弯曲构象延伸到延伸构象的机械能垒的描述。使用不同的基质杨氏模量对整合素聚集动力学进行了一系列的蒙特卡洛模拟,这表明,一旦它们开始在刚度阈值之上组装,就会有更多的整合素聚集在较硬的基底上,表明粘附核对基底弹性的响应性是与先前报告的结果合理吻合。同样,这些模拟表明整联蛋白簇对底物刚度的敏感性是通过受体-配体对之间的化学亲和力和通过衔接蛋白交联的整联蛋白之间的亲和力以及细胞膜上整联蛋白的密度介导的。该研究提供了有关整合素介导的细胞基质初始黏附的机械感测内在机制的迷人见解。

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