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Tissue-specific mechanical and geometrical control of cell viability and actin cytoskeleton alignment

机译:细胞活力和肌动蛋白细胞骨架排列的组织特异性机械和几何控制

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摘要

Different tissues have specific mechanical properties and cells of different geometries, such as elongated muscle cells and polygonal endothelial cells, which are precisely regulated during embryo development. However, the mechanisms that underlie these processes are not clear. Here, we built an in vitro model to mimic the cellular microenvironment of muscle by combining both mechanical stretch and geometrical control. We found that mechanical stretch was a key factor that determined the optimal geometry of myoblast C2C12 cells under stretch, whereas vascular endothelial cells and fibroblasts had no such dependency. We presented the first experimental evidence that can explain why myoblasts are destined to take the elongated geometry so as to survive and maintain parallel actin filaments along the stretching direction. The study is not only meaningful for the research on myogenesis but also has potential application in regenerative medicine.
机译:不同的组织具有特定的机械特性,并且具有不同几何形状的细胞(例如细长的肌肉细胞和多边形内皮细胞)在胚胎发育过程中受到精确调节。但是,这些过程的基础机制尚不清楚。在这里,我们建立了一个体外模型,通过结合机械拉伸和几何控制来模拟肌肉的细胞微环境。我们发现机械拉伸是决定拉伸下成肌细胞C2C12细胞最佳几何形状的关键因素,而血管内皮细胞和成纤维细胞则没有这种依赖性。我们提出了第一个实验证据,可以解释为什么成肌细胞注定要采取细长的几何形状,以便在拉伸方向上存活并保持平行的肌动蛋白丝。该研究不仅对肌发生的研究具有重要意义,而且在再生医学中具有潜在的应用前景。

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