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Geometric control of cell life and death

机译:细胞生命和死亡的几何控制

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Human and bovine capillary endothelial cells were switched from growth to apoptosis by using micropatterned substrates that contained extracellular matrix-coated adhesive islands of decreasing size to progressively restrict cell extension. Cell spreading also was varied while maintaining the total cell-matrix contact area constant by changing the spacing between multiple focal adhesion-sized islands. Cell shape was found to govern whether individual cells grow or die, regardless of the type of matrix protein or antibody to integrin used to mediate adhesion. Local geometric control of cell growth and viability may therefore represent a fundamental mechanism for developmental regulation within the tissue microenvironment.
机译:人类和牛毛细血管内皮细胞通过使用微图案化的底物从生长切换到凋亡,该底物包含大小减小的细胞外基质涂层粘附岛,从而逐渐限制细胞的延伸。通过改变多个粘着斑大小的岛之间的间隔,在保持总细胞-基质接触面积恒定的同时,细胞扩散也发生了变化。发现细胞形状决定着单个细胞的生长还是死亡,而与基质蛋白或用于介导粘附的整联蛋白抗体的类型无关。因此,细胞生长和活力的局部几何控制可能代表了组织微环境内发育调节的基本机制。

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