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整合素胞质结构域相关蛋白-1α对粘着斑的破坏作用

Disruption of focal adhesions by integrin cytoplasmic domain-associated protein-1 alpha.

作者信息

Bouvard Daniel, Vignoud Lucile, Dupé-Manet Sandra, Abed Nadia, Fournier Henri-Noël, Vincent-Monegat Carole, Retta Saverio Francesco, Fassler Reinhard, Block Marc R

机构信息

Laboratoire d'Etude de la Differenciation et de l'Adhérence Cellulaires, Unité Mixte de Recherche UJF/CNRS 5538, Institut Albert Bonniot, Faculte de Médecine de Grenoble, La Tronche F38706 cedex, France.

出版信息

J Biol Chem. 2003 Feb 21;278(8):6567-74. doi: 10.1074/jbc.M211258200. Epub 2002 Dec 7.

Abstract

Regulation of integrin affinity and clustering plays a key role in the control of cell adhesion and migration. The protein ICAP-1 alpha (integrin cytoplasmic domain-associated protein-1 alpha) binds to the cytoplasmic domain of the beta(1A) integrin and controls cell spreading on fibronectin. Here, we demonstrate that, despite its ability to interact with beta(1A) integrin, ICAP-1 alpha is not recruited in focal adhesions, whereas it is colocalized with the integrin at the ruffling edges of the cells. ICAP-1 alpha induced a rapid disruption of focal adhesions, which may result from the ability of ICAP-1 alpha to inhibit the association of beta(1A) integrin with talin, which is crucial for the assembly of these structures. ICAP-1 alpha-mediated dispersion of beta(1A) integrins is not observed with beta(1D) integrins that do not bind ICAP. This strongly suggests that ICAP-1 alpha action depends on a direct interaction between ICAP-1 alpha and the cytoplasmic domain of the beta(1) chains. Altogether, these results suggest that ICAP-1 alpha plays a key role in cell adhesion by acting as a negative regulator of beta(1) integrin avidity.

摘要

整合素亲和力和聚集的调节在细胞黏附和迁移的控制中起着关键作用。蛋白ICAP-1α(整合素胞质结构域相关蛋白-1α)与β(1A)整合素的胞质结构域结合,并控制细胞在纤连蛋白上的铺展。在此,我们证明,尽管ICAP-1α具有与β(1A)整合素相互作用的能力,但它并不定位于粘着斑,而是与整合素在细胞的边缘褶边处共定位。ICAP-1α诱导粘着斑迅速解体,这可能是由于ICAP-1α抑制β(1A)整合素与踝蛋白结合的能力所致,而踝蛋白对于这些结构的组装至关重要。对于不与ICAP结合的β(1D)整合素,未观察到ICAP-1α介导的β(1A)整合素的分散。这强烈表明ICAP-1α的作用取决于ICAP-1α与β(1)链胞质结构域之间的直接相互作用。总之,这些结果表明ICAP-1α作为β(1)整合素亲和力的负调节因子,在细胞黏附中起关键作用。

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