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肌动蛋白逆行流主动排列并调整粘着斑中配体结合的整合素。

Actin retrograde flow actively aligns and orients ligand-engaged integrins in focal adhesions.

机构信息

Whitman Center, Marine Biological Laboratory, Woods Hole, MA 02543.

Physiology Course, Marine Biological Laboratory, Woods Hole, MA 02543.

出版信息

Proc Natl Acad Sci U S A. 2017 Oct 3;114(40):10648-10653. doi: 10.1073/pnas.1701136114.

Abstract

Integrins are transmembrane receptors that, upon activation, bind extracellular ligands and link them to the actin filament (F-actin) cytoskeleton to mediate cell adhesion and migration. Cytoskeletal forces in migrating cells generated by polymerization- or contractility-driven "retrograde flow" of F-actin from the cell leading edge have been hypothesized to mediate integrin activation for ligand binding. This predicts that these forces should align and orient activated, ligand-bound integrins at the leading edge. Here, polarization-sensitive fluorescence microscopy of GFP-αVβ3 integrins in fibroblasts shows that integrins are coaligned in a specific orientation within focal adhesions (FAs) in a manner dependent on binding immobilized ligand and a talin-mediated linkage to the F-actin cytoskeleton. These findings, together with Rosetta modeling, suggest that integrins in FA are coaligned and may be highly tilted by cytoskeletal forces. Thus, the F-actin cytoskeleton sculpts an anisotropic molecular scaffold in FAs, and this feature may underlie the ability of migrating cells to sense directional extracellular cues.

摘要

整合素是一种跨膜受体,在被激活后,它会与细胞外配体结合,并将它们与肌动蛋白丝(F-actin)细胞骨架连接起来,从而介导细胞黏附和迁移。迁移细胞中的细胞骨架力是由 F-actin 从细胞前缘的聚合或收缩驱动的“逆行流动”产生的,据推测,这些力可以介导整合素的激活,从而与配体结合。这表明这些力应该在前沿对齐并定向激活、配体结合的整合素。在这里,对成纤维细胞中 GFP-αVβ3 整合素的偏振敏感荧光显微镜显示,整合素在黏附斑(FAs)中以特定的方向共定位,这种方式依赖于与固定化配体的结合以及与 F-actin 细胞骨架的 talin 介导的连接。这些发现,结合 Rosetta 建模,表明 FA 中的整合素是共定位的,并且可能受到细胞骨架力的强烈倾斜。因此,F-actin 细胞骨架在 FA 中塑造了一个各向异性的分子支架,而这一特征可能是迁移细胞感知定向细胞外线索的能力的基础。

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