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关于底物曲率对细胞力学的影响。

On the effect of substrate curvature on cell mechanics.

作者信息

Sanz-Herrera José A, Moreo Pedro, García-Aznar José M, Doblaré Manuel

机构信息

Group of Structural Mechanics and Materials Modeling, Aragón Institute of Engineering Research (I3A), Universidad de Zaragoza, Torres Quevedo Building, 50018 Zaragoza, Spain.

出版信息

Biomaterials. 2009 Dec;30(34):6674-86. doi: 10.1016/j.biomaterials.2009.08.053. Epub 2009 Sep 24.

Abstract

Cell movement on a substrate or within the extracellular matrix is the phenomenological response to a biochemical signals' cascade transcripted into biophysical processes and viceversa. The process is complex in nature, including different length scales from the whole cell to organelle and protein levels, where substrate/ECM curvature has been shown to play an important role on cell's behavior. From a macroscopic perspective, the cytoskeleton may be modeled as a continuum body unbalanced by internal protein motors. In this work, we propose a cell constitutive model to simulate cell attachment on curved substrates, activated by contractile forces. We first analyze a single fiber bundle composed by microtubules, actin filaments and myosin machinery. Then, the model is macroscopically extended to the cytoskeletal level using homogenization. Substrate curvature has two implications in our model: (i) it forces fibers to work in a curved (bent) position and (ii) it eventually creates a pre-deformation state in the cytoskeleton. Interestingly, the model shows higher contractile force inhibition as curvature increases when implemented over different substrate morphologies, being this consistent with experimental results. The presented model may result useful in many new regenerative medicine techniques, miniaturized experimental tests, or to analyze cell behavior on manufactured nanoscaffolds for tissue engineering.

摘要

细胞在基质上或细胞外基质内的运动是对转录为生物物理过程的生化信号级联的现象学响应,反之亦然。该过程本质上很复杂,包括从整个细胞到细胞器和蛋白质水平的不同长度尺度,其中已表明基质/细胞外基质的曲率对细胞行为起着重要作用。从宏观角度来看,细胞骨架可被建模为一个由内部蛋白质马达驱动的不平衡连续体。在这项工作中,我们提出了一个细胞本构模型,以模拟由收缩力激活的细胞在弯曲基质上的附着。我们首先分析由微管、肌动蛋白丝和肌球蛋白机制组成的单纤维束。然后,使用均匀化方法将该模型宏观扩展到细胞骨架水平。基质曲率在我们的模型中有两个影响:(i)它迫使纤维在弯曲位置工作,(ii)它最终在细胞骨架中产生一个预变形状态。有趣的是,当在不同的基质形态上实施时,该模型显示随着曲率增加收缩力抑制作用增强,这与实验结果一致。所提出的模型可能在许多新的再生医学技术、小型化实验测试或分析用于组织工程的人造纳米支架上的细胞行为方面很有用。

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