Src Kinase Activation by Direct Interaction with the Integrin Beta Cytoplasmic Domain

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2003 Nov 1

PMID 14593208

Citations 252

Authors

Elena G Arias-Salgado

Sergio Lizano

Sugata Sarkar

Joan S Brugge

Mark H Ginsberg

Sanford J Shattil

Affiliations

Soon will be listed here.

Abstract

Src tyrosine kinases transmit integrin-dependent signals pivotal for cell movement and proliferation. Here, we establish a mechanism for Src activation by integrins. c-Src is shown to bind constitutively and selectively to beta3 integrins through an interaction involving the c-Src SH3 domain and the carboxyl-terminal region of the beta3 cytoplasmic tail. Clustering of beta3 integrins in vivo activates c-Src and induces phosphorylation of Tyr-418 in the c-Src activation loop, a reaction essential for adhesion-dependent phosphorylation of Syk, a c-Src substrate. Unlike c-Src, Hck, Lyn, and c-Yes bind more generally to beta1A, beta2, and beta3 cytoplasmic tails. These results invoke a model whereby Src is primed for activation by direct interaction with an integrin beta tail, and integrin clustering stabilizes activated Src by inducing intermolecular autophosphorylation. The data provide a paradigm for integrin regulation of Src and a molecular basis for the similar functional defects of osteoclasts or platelets from mice lacking beta3 integrins or c-Src.

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