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Rac1 Recruitment to the Archipelago Structure of the Focal Adhesion through the Fluid Membrane as Revealed by Single-Molecule Analysis

机译:Rac1招募通过分子膜的粘着力通过分子膜的群岛粘附的群岛结构。

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摘要

The focal adhesion (FA) is an integrin-based structure built in/on the plasma membrane (PM), linking the extracellular matrix to the actin stress-fibers, working as cell migration scaffolds. Previously, we proposed the archipelago architecture of the FA, in which FA largely consists of fluid membrane, dotted with small islands accumulating FA proteins: membrane molecules enter the inter-island channels in the FA zone rather freely, and the integrins in the FA-protein islands rapidly exchanges with those in the bulk membrane. Here, we examined how Rac1, a small G-protein regulating FA formation, and its activators αPIX and βPIX, are recruited to the FA zones. PIX molecules are recruited from the cytoplasm to the FA zones directly. In contrast, majorities of Rac1 molecules first arrive from the cytoplasm on the general inner PM surface, and then enter the FA zones via lateral diffusion on the PM, which is possible due to rapid Rac1 diffusion even within the FA zones, slowed only by a factor of two to four compared with that outside. The constitutively-active Rac1 mutant exhibited temporary and all-time immobilizations in the FA zone, suggesting that upon PIX-induced Rac1 activation at the FA-protein islands, Rac1 tends to be immobilized at the FA-protein islands. © 2013 Wiley Periodicals, Inc
机译:粘着斑(FA)是一种构建在质膜(PM)内/上的基于整联蛋白的结构,将细胞外基质与肌动蛋白应力纤维相连,充当细胞迁移的支架。先前,我们提出了FA的群岛架构,其中FA主要由流体膜组成,点缀着小岛上积累的FA蛋白:膜分子相当自由地进入FA区的岛间通道,而FA中的整联蛋白蛋白质岛与主体膜中的蛋白质岛快速交换。在这里,我们研究了如何调节FA形成的小G蛋白Rac1及其激活剂αPIX和βPIX被募集到FA区域。 PIX分子直接从细胞质募集到FA区。相比之下,大多数Rac1分子首先从一般内PM表面的细胞质到达,然后通过PM上的侧向扩散进入FA区,这可能是由于Rac1快速扩散,即使在FA区内也是如此,只有通过与外界相比,是二至四倍。组成型活性Rac1突变体在FA区域表现出暂时性和长期固定性,表明在PIX诱导的FAac蛋白岛上激活Rac1后,Rac1倾向于固定在FA蛋白岛上。 ©2013 Wiley Periodicals,Inc

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