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JCS ePress online publication date 28 Oct 2008
doi: 10.1242/jcs.028423


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Research Article

A dual role for caveolin-1 in the regulation of fibronectin matrix assembly by uPAR


Elizabeth Monaghan-Benson, Cynthia Corley Mastick, and Paula J. McKeown-Longo*
* Author for correspondence (e-mail: mckeowp{at}mail.amc.edu)

The relationship between the plasminogen activator system and integrin function is well documented but incompletely understood. The mechanism of uPAR-mediated signaling across the membrane and the molecular basis of uPAR-dependent activation of integrins remain important issues. The present study was undertaken to identify the molecular intermediates involved in the uPAR signaling pathway controlling {alpha}5{beta}1-integrin activation and fibronectin polymerization. Disruption of lipid rafts with M{beta}CD or depletion of caveolin-1 by siRNA led to the inhibition of uPAR-dependent integrin activation and stimulation of fibronectin polymerization in human dermal fibroblasts. The data indicate a dual role for caveolin-1 in the uPAR signaling pathway, leading to integrin activation. Caveolin-1 functions initially as a membrane adaptor or scaffold to mediate uPAR-dependent activation of Src and EGFR. Subsequently, in its phosphorylated form, caveolin-1 acts as an accessory molecule to direct trafficking of activated EGFR to focal adhesions. These studies provide a novel paradigm for the regulation of crosstalk among integrins, growth-factor receptors and uPAR.


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© The Company of Biologists Ltd 2008