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整合素α4-14-3-3ζ-桩蛋白三元复合物介导局部Cdc42活性并加速细胞迁移。

An integrin-alpha4-14-3-3zeta-paxillin ternary complex mediates localised Cdc42 activity and accelerates cell migration.

作者信息

Deakin Nicholas O, Bass Mark D, Warwood Stacey, Schoelermann Julia, Mostafavi-Pour Zohreh, Knight David, Ballestrem Christoph, Humphries Martin J

机构信息

Wellcome Trust Centre for Cell-Matrix Research, Faculty of Life Sciences, University of Manchester, Oxford Road, Manchester M13 9PT, UK.

出版信息

J Cell Sci. 2009 May 15;122(Pt 10):1654-64. doi: 10.1242/jcs.049130. Epub 2009 Apr 28.

Abstract

Alpha4 integrins are used by leukocytes and neural crest derivatives for adhesion and migration during embryogenesis, immune responses and tumour invasion. The pro-migratory activity of alpha4 integrin is mediated in part through the direct binding of the cytoplasmic domain to paxillin. Here, using intermolecular FRET and biochemical analyses, we report a novel interaction of the alpha4 integrin cytoplasmic domain with 14-3-3zeta. This interaction depends on serine phosphorylation of alpha4 integrin at a site (S978) distinct from that which regulates paxillin binding (S988). Using a combination of metabolic labelling and targeted mass spectrometry by multiple reaction monitoring we demonstrate the low stoichiometry phosphorylation of S978. The interaction between alpha4 integrin and 14-3-3zeta is enhanced by the direct association between 14-3-3zeta and paxillin, resulting in the formation of a ternary complex that stabilises the recruitment of each component. Although pair-wise interaction between alpha4 integrin and paxillin is sufficient for normal Rac1 regulation, the integrity of the ternary complex is essential for focused Cdc42 activity at the lamellipodial leading edge and directed cell movement. Taken together, these data identify a key signalling nexus mediating alpha4 integrin-dependent migration.

摘要

α4整合素在胚胎发育、免疫反应和肿瘤侵袭过程中被白细胞和神经嵴衍生物用于黏附和迁移。α4整合素的促迁移活性部分是通过其胞质结构域与桩蛋白的直接结合来介导的。在此,我们利用分子间荧光共振能量转移和生化分析,报告了α4整合素胞质结构域与14-3-3ζ的一种新相互作用。这种相互作用依赖于α4整合素在一个与调节桩蛋白结合的位点(S988)不同的位点(S978)上的丝氨酸磷酸化。通过代谢标记和多反应监测靶向质谱联用,我们证明了S978的低化学计量磷酸化。14-3-3ζ与桩蛋白的直接结合增强了α4整合素与14-3-3ζ之间的相互作用,导致形成一个三元复合物,该复合物稳定了每个组分的募集。虽然α4整合素与桩蛋白之间的两两相互作用足以正常调节Rac1,但三元复合物的完整性对于片状伪足前沿聚焦的Cdc42活性和定向细胞运动至关重要。综上所述,这些数据确定了一个介导α4整合素依赖性迁移的关键信号枢纽。

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