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整合素细胞质结构域相关蛋白1的核转位刺激细胞增殖。

Nuclear translocation of integrin cytoplasmic domain-associated protein 1 stimulates cellular proliferation.

作者信息

Fournier Henri-Noël, Dupé-Manet Sandra, Bouvard Daniel, Luton Frédéric, Degani Simona, Block Marc R, Retta Saverio Francesco, Albiges-Rizo Corinne

机构信息

Laboratoire d'Etude de la Différenciation et de l'Adhérence Cellulaires, Unité Mixte Recherche Université Joseph Fourier/Centre National de la Recherche Scientifique 5538 Institut Albert Bonniot, Faculté de Médecine de Grenoble, La Tronche Cedex, France.

出版信息

Mol Biol Cell. 2005 Apr;16(4):1859-71. doi: 10.1091/mbc.e04-08-0744. Epub 2005 Feb 9.

Abstract

Integrin cytoplasmic domain-associated protein 1 (ICAP-1) has been shown to interact specifically with the beta1 integrin cytoplasmic domain and to control cell spreading on fibronectin. Interestingly, ICAP-1 also is observed in the nucleus, by immunocytochemical staining, and after biochemical cell fractionation, suggesting that it has additional roles that have yet to be determined. We show that the nucleocytoplasmic shuttling capability of ICAP-1 is dependent on a functional nuclear localization signal. In addition, overexpression of beta1 integrin strongly reduced this nuclear localization, suggesting that integrin activity could modulate ICAP-1 shuttling by sequestering it in the cytoplasm. Indeed, the nuclear localization of ICAP-1 is dependent on the stage of cell spreading on fibronectin, and we also show that ICAP-1 expression stimulates cellular proliferation in a fibronectin-dependent manner. This function is dependent on its nuclear localization. Moreover, ICAP-1 is able to activate the c-myc promoter in vitro. Together, these results demonstrate that ICAP-1 shuttles between the nucleus and cytoplasm in a beta1 integrin-dependent manner. It could act as a messenger that relays information from sites of integrin-dependent cell adhesion to the nucleus for controlling gene expression and cell proliferation.

摘要

整合素胞质结构域相关蛋白1(ICAP-1)已被证明能与β1整合素胞质结构域特异性相互作用,并控制细胞在纤连蛋白上的铺展。有趣的是,通过免疫细胞化学染色以及生化细胞分级分离,在细胞核中也观察到了ICAP-1,这表明它还有尚未确定的其他作用。我们发现ICAP-1的核质穿梭能力依赖于一个功能性核定位信号。此外,β1整合素的过表达强烈降低了这种核定位,这表明整合素活性可能通过将ICAP-1隔离在细胞质中来调节其穿梭。事实上,ICAP-1的核定位依赖于细胞在纤连蛋白上的铺展阶段,并且我们还表明ICAP-1的表达以纤连蛋白依赖的方式刺激细胞增殖。该功能依赖于其核定位。此外,ICAP-1能够在体外激活c-myc启动子。总之,这些结果表明ICAP-1以β1整合素依赖的方式在细胞核和细胞质之间穿梭。它可能作为一种信使,将来自整合素依赖的细胞黏附位点的信息传递到细胞核,以控制基因表达和细胞增殖。

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