AXL confers cell migration and invasion by hijacking a PEAK1-regulated focal adhesion protein network

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作者
Afnan Abu-Thuraia
Marie-Anne Goyette
Jonathan Boulais
Carine Delliaux
Chloé Apcher
Céline Schott
Rony Chidiac
Halil Bagci
Marie-Pier Thibault
Dominique Davidson
Mathieu Ferron
André Veillette
Roger J. Daly
Anne-Claude Gingras
Jean-Philippe Gratton
Jean-François Côté
机构
[1] Montreal Clinical Research Institute (IRCM),Molecular Biology Programs
[2] Université de Montréal,Department of Pharmacology and Physiology
[3] Université de Montréal,Department of Anatomy and Cell Biology
[4] McGill University,Division of Experimental Medicine
[5] McGill University,Cancer Program, Biomedicine Discovery Institute and Department of Biochemistry and Molecular Biology
[6] Monash University,Lunenfeld
[7] Sinai Health System,Tanenbaum Research Institute
[8] University of Toronto,Department of Molecular Genetics
[9] Université de Montréal,Department of Biochemistry and Molecular Medicine
[10] ETH Zürich,Institute of Biochemistry
来源
Nature Communications | / 11卷
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摘要
Aberrant expression of receptor tyrosine kinase AXL is linked to metastasis. AXL can be activated by its ligand GAS6 or by other kinases, but the signaling pathways conferring its metastatic activity are unknown. Here, we define the AXL-regulated phosphoproteome in breast cancer cells. We reveal that AXL stimulates the phosphorylation of a network of focal adhesion (FA) proteins, culminating in faster FA disassembly. Mechanistically, AXL phosphorylates NEDD9, leading to its binding to CRKII which in turn associates with and orchestrates the phosphorylation of the pseudo-kinase PEAK1. We find that PEAK1 is in complex with the tyrosine kinase CSK to mediate the phosphorylation of PAXILLIN. Uncoupling of PEAK1 from AXL signaling decreases metastasis in vivo, but not tumor growth. Our results uncover a contribution of AXL signaling to FA dynamics, reveal a long sought-after mechanism underlying AXL metastatic activity, and identify PEAK1 as a therapeutic target in AXL positive tumors.
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