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Sos-1协调Ras和Rac激活的机制。

Mechanisms through which Sos-1 coordinates the activation of Ras and Rac.

作者信息

Innocenti Metello, Tenca Pierluigi, Frittoli Emanuela, Faretta Mario, Tocchetti Arianna, Di Fiore Pier Paolo, Scita Giorgio

机构信息

Department of Experimental Oncology, European Institute of Oncology, Via Ripamonti, 435, 20141 Milan, Italy.

出版信息

J Cell Biol. 2002 Jan 7;156(1):125-36. doi: 10.1083/jcb.200108035. Epub 2002 Jan 3.

Abstract

Signaling from receptor tyrosine kinases (RTKs)* requires the sequential activation of the small GTPases Ras and Rac. Son of sevenless (Sos-1), a bifunctional guanine nucleotide exchange factor (GEF), activates Ras in vivo and displays Rac-GEF activity in vitro, when engaged in a tricomplex with Eps8 and E3b1-Abi-1, a RTK substrate and an adaptor protein, respectively. A mechanistic understanding of how Sos-1 coordinates Ras and Rac activity is, however, still missing. Here, we demonstrate that (a) Sos-1, E3b1, and Eps8 assemble into a tricomplex in vivo under physiological conditions; (b) Grb2 and E3b1 bind through their SH3 domains to the same binding site on Sos-1, thus determining the formation of either a Sos-1-Grb2 (S/G) or a Sos-1-E3b1-Eps8 (S/E/E8) complex, endowed with Ras- and Rac-specific GEF activities, respectively; (c) the Sos-1-Grb2 complex is disrupted upon RTKs activation, whereas the S/E/E8 complex is not; and (d) in keeping with the previous result, the activation of Ras by growth factors is short-lived, whereas the activation of Rac is sustained. Thus, the involvement of Sos-1 at two distinct and differentially regulated steps of the signaling cascade allows for coordinated activation of Ras and Rac and different duration of their signaling within the cell.

摘要

受体酪氨酸激酶(RTKs)*发出的信号需要小GTP酶Ras和Rac的顺序激活。七号less之子(Sos-1)是一种双功能鸟嘌呤核苷酸交换因子(GEF),在体内激活Ras,并在体外与Eps8和E3b1-Abi-1分别形成三聚体复合物时显示出Rac-GEF活性,Eps8是一种RTK底物,E3b1-Abi-1是一种衔接蛋白。然而,对于Sos-1如何协调Ras和Rac活性的机制仍不清楚。在这里,我们证明:(a)在生理条件下,Sos-1、E3b1和Eps8在体内组装成三聚体复合物;(b)Grb2和E3b1通过它们的SH3结构域结合到Sos-1上的相同结合位点,从而分别决定形成具有Ras特异性GEF活性的Sos-1-Grb2(S/G)复合物或具有Rac特异性GEF活性的Sos-1-E3b1-Eps8(S/E/E8)复合物;(c)RTKs激活后,Sos-1-Grb2复合物被破坏,而S/E/E8复合物未被破坏;(d)与先前的结果一致,生长因子对Ras的激活是短暂的,而对Rac的激活是持续的。因此,Sos-1参与信号级联的两个不同且受不同调节的步骤,使得Ras和Rac能够协同激活,并在细胞内具有不同的信号持续时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ad81/2173577/eb8cfd83ba8c/0108035f1.jpg

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