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Crawling from soft to stiff matrix polarizes the cytoskeleton and phosphoregulates myosin-II heavy chain

机译:从软基质到硬基质的爬行会使细胞骨架极化并使肌球蛋白-II重链磷酸化

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摘要

On rigid surfaces, the cytoskeleton of migrating cells is polarized, but tissue matrix is normally soft. We show that nonmuscle MIIB (myosin-IIB) is unpolarized in cells on soft matrix in 2D and also within soft 3D collagen, with rearward polarization of MIIB emerging only as cells migrate from soft to stiff matrix. Durotaxis is the tendency of cells to crawl from soft to stiff matrix, and durotaxis of primary mesenchymal stem cells (MSCs) proved more sensitive to MIIB than to the more abundant and persistently unpolarized nonmuscle MIIA (myosin-IIA). However, MIIA has a key upstream role: in cells on soft matrix, MIIA appeared diffuse and mobile, whereas on stiff matrix, MIIA was strongly assembled in oriented stress fibers that MIIB then polarized. The difference was caused in part by elevated phospho-S1943–MIIA in MSCs on soft matrix, with site-specific mutants revealing the importance of phosphomoderated assembly of MIIA. Polarization is thus shown to be a highly regulated compass for mechanosensitive migration.
机译:在刚性表面上,迁移细胞的细胞骨架是极化的,但组织基质通常较软。我们显示,非肌肉MIIB(肌球蛋白IIB)在2D以及在软3D胶原内的软基质上的细胞中都是非极化的,MIIB的向后极化仅在细胞从软基质迁移到硬基质时才出现。 Durotaxis是细胞从软基质爬行到刚性基质的趋势,并且事实证明,原代间充质干细胞(MSCs)的durotaxis对MIIB的敏感性高于对更丰富且持续极化的非肌肉MIIA(肌球蛋白IIA)的敏感性。但是,MIIA具有关键的上游作用:在软基质上的细胞中,MIIA出现扩散且活动,而在硬基质上,MIIA牢固地组装在取向应力纤维中,然后MIIB极化。造成这种差异的部分原因是软基质上的MSC中的磷酸S1943-MIIA升高,位点特异性突变体揭示了磷酸化MIIA组装的重要性。因此,显示极化是机械敏感迁移的高度受控的指南针。

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