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Fluctuations of intracellular forces during cell protrusion

机译:细胞突出过程中细胞内力的波动

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摘要

We propose a model to infer from live cell images of actin filament (F-actin) flow intracellular force variations during protrusion-retraction cycles of epithelial cells in a wound healing response. To establish mechanistic relations between force development and cytoskeleton dynamics, force fluctuations were correlated with fluctuations in F-actin turnover, flow, and F-actin-vinculin coupling. Our analyses suggest that force transmission at focal adhesions (FA) requires binding of vinculin to F-actin and integrin (indirectly), which is modulated at the vinculin-integrin but not the vinculin-F-actin interface. Force transmission at FAs is co-localized in space and synchronized in time with transient increases of the boundary force at the cell edge. Surprisingly, the maxima in adhesion and boundary forces lag maximal edge advancement by ∼40 s. Maximal F-actin assembly is observed ∼20 s after maximal edge advancement. Based on these findings, we propose that protrusion events are limited by membrane tension and that the characteristic duration of a protrusion cycle is determined by the efficiency in reinforcing F-actin assembly and adhesion formation as tension increases.
机译:我们提出一个模型,从上皮细胞在伤口愈合反应中的上缩回缩周期中肌动蛋白丝(F-肌动蛋白)流动的活细胞图像推断细胞内力变化。为了建立力发展和细胞骨架动力学之间的机械关系,力波动与F-肌动蛋白周转,流量和F-肌动蛋白-维库林偶联的波动相关。我们的分析表明,在粘着斑(FA)处的力传递需要将纽蛋白与F-肌动蛋白和整联蛋白(间接)结合,后者在纽蛋白-整联蛋白而不是纽蛋白-F-肌动蛋白的界面上被调节。 FA处的力传递在空间中共定位,并且在时间上与单元边缘的边界力的瞬时增加同步。出人意料的是,粘附力和边界力的最大值比最大边缘前进滞后约40 s。最大边缘推进后约20 s观察到最大的F-肌动蛋白装配。基于这些发现,我们提出突出事件受到膜张力的限制,并且突出循环的特征持续时间由随着张力增加而增强F-肌动蛋白组装和粘附形成的效率决定。

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  • 期刊名称 other
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  • 年(卷),期 -1(10),12
  • 年度 -1
  • 页码 1393–1400
  • 总页数 19
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