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Syndecan-1 controls cell migration by activating Rap1 to regulate focal adhesion disassembly.


ABSTRACT: After injury, residual epithelial cells coordinate contextual clues from cell-cell and cell-matrix interactions to polarize and migrate over the wound bed. Protrusion formation, cell body translocation and rear retraction is a repetitive process that allows the cell to move across the substratum. Fundamental to this process is the assembly and disassembly of focal adhesions that facilitate cell adhesion and protrusion formation. Here, we identified syndecan-1 as a regulator of focal adhesion disassembly in migrating lung epithelial cells. Syndecan-1 altered the dynamic exchange of adhesion complex proteins, which in turn regulates migration speed. Moreover, we provide evidence that syndecan-1 controls this entire process through Rap1. Thus, syndecan-1 restrains migration in lung epithelium by activating Rap1 to slow focal adhesion disassembly.

SUBMITTER: Altemeier WA 

PROVIDER: S-EPMC3533394 | biostudies-literature | 2012 Nov

REPOSITORIES: biostudies-literature

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Syndecan-1 controls cell migration by activating Rap1 to regulate focal adhesion disassembly.

Altemeier William A WA   Schlesinger Saundra Y SY   Buell Catherine A CA   Parks William C WC   Chen Peter P  

Journal of cell science 20120816 Pt 21


After injury, residual epithelial cells coordinate contextual clues from cell-cell and cell-matrix interactions to polarize and migrate over the wound bed. Protrusion formation, cell body translocation and rear retraction is a repetitive process that allows the cell to move across the substratum. Fundamental to this process is the assembly and disassembly of focal adhesions that facilitate cell adhesion and protrusion formation. Here, we identified syndecan-1 as a regulator of focal adhesion dis  ...[more]

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