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SRC-3Delta4 mediates the interaction of EGFR with FAK to promote cell migration.


ABSTRACT: EGF induces signal transduction between EGFR and FAK, and FAK is required for EGF-induced cell migration. It is unknown, however, what factor mediates the interaction between EGFR and FAK and leads to EGF-induced FAK phosphorylation. Here, we identify SRC-3Delta4, a splicing isoform of the SRC-3 oncogene, as a signaling adaptor that links EGFR and FAK and promotes EGF-induced phosphorylations of FAK and c-Src. We identify three PAK1-mediated phosphorylations in SRC-3Delta4 that promote the localization of SRC-3Delta4 to the plasma membrane and mediate the interactions with EGFR and FAK. Importantly, overexpression of SRC-3Delta4 promotes MDA-MB231-induced breast tumor metastasis. Our findings identify phosphorylated SRC-3Delta4 as a missing adaptor between EGFR and its downstream signaling molecule FAK to coordinately regulate EGF-induced cell migration. Our study also reveals that a nuclear receptor coactivator can act in the periphery of a cell to directly mediate activation of an enzyme.

SUBMITTER: Long W 

PROVIDER: S-EPMC2824333 | biostudies-literature | 2010 Feb

REPOSITORIES: biostudies-literature

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SRC-3Delta4 mediates the interaction of EGFR with FAK to promote cell migration.

Long Weiwen W   Yi Ping P   Amazit Larbi L   LaMarca Heather L HL   Ashcroft Felicity F   Kumar Rakesh R   Mancini Michael A MA   Tsai Sophia Y SY   Tsai Ming-Jer MJ   O'Malley Bert W BW  

Molecular cell 20100201 3


EGF induces signal transduction between EGFR and FAK, and FAK is required for EGF-induced cell migration. It is unknown, however, what factor mediates the interaction between EGFR and FAK and leads to EGF-induced FAK phosphorylation. Here, we identify SRC-3Delta4, a splicing isoform of the SRC-3 oncogene, as a signaling adaptor that links EGFR and FAK and promotes EGF-induced phosphorylations of FAK and c-Src. We identify three PAK1-mediated phosphorylations in SRC-3Delta4 that promote the local  ...[more]

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