GIT1 Mediates VEGF-Induced Podosome Formation in Endothelial Cells: Critical Role for PLC{gamma}

doi:10.1161/ATVBAHA.108.174391

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Arteriosclerosis, Thrombosis, and Vascular Biology. 2009;29:202-208
Published online before print November 20, 2008, doi: 10.1161/ATVBAHA.108.174391

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GIT1 Mediates VEGF-Induced Podosome Formation in Endothelial Cells

Critical Role for PLC ${gamma}$

Jing Wang; Yoji Taba; Jinjiang Pang; Guoyong Yin; Chen Yan; Bradford C. Berk

From the Aab Cardiovascular Research Institute and Department of Medicine, University of Rochester School of Medicine and Dentistry, NY.

Correspondence to Bradford Berk, MD, PhD, University of Rochester, Box 706, Aab Cardiovascular Research Institute, 601 Elmwood Ave, Rochester, NY 14642. E-mail Bradford_Berk{at}urmc.rochester.edu

Objective— We and others showed that tyrosine kinase receptors(TKRs) such as the epidermal growth factor receptor stimulateG protein-coupled receptor (GPCR) kinase-interacting protein1 (GIT1) phosphorylation via c-Src, which is required for phospholipaseC- ${gamma}$ (PLC ${gamma}$ ) activation, indicating that GIT1 participates in TKRsignaling. VEGF is the most important TKR in endothelial cells(ECs); essential for cell survival, migration, and angiogenesis.Podosomes, actin-rich structures, were found to contribute toEC migration, tissue invasion, and matrix remodeling, suggestinga role for podosomes in angiogenesis. Because GIT1 is a substrateof c-Src, and podosome formation is c-Src dependent, we hypothesizedthat GIT1 plays an important role in VEGF-induced EC podosomeformation and cell migration.

Methods and Results— Exposure of ECs to VEGF for 30 minutesstimulated GIT1 colocalization with podosomes. Depletion ofGIT1 by siRNA significantly decreased VEGF-induced podosomeformation. A key role for PLC ${gamma}$ was suggested by several experiments.Double staining PLC ${gamma}$ and actin showed colocalization of PLC ${gamma}$ withpodosomes. Podosome formation was dramatically reduced by PLC ${gamma}$ inhibitor U73122, Src inhibitor PP2, or expression of dominantnegative small GTPases. Therefore, VEGF-induced EC podosomeformation is dependent on Src, GIT1, PLC ${gamma}$ , and small GTPases.In addition, matrix metalloprotease 2 (MMP2) and MT-MMP1 weredetected at sites of VEGF-induced podosomes. Depletion of GIT1by siRNA also significantly inhibited VEGF-induced MMP2 activationand extracellular matrix (ECM) degradation. Therefore, GIT1mediates VEGF-induced matrix metalloproteinase (MMP) activationand ECM degradation by regulating podosome formation. Finally,depletion of GIT1 by siRNA significantly decreased VEGF-inducedcell migration.

Conclusions— These data indicate that GIT1 is an essentialmediator for VEGF-induced EC podosome formation and cell migrationvia PLC ${gamma}$ .

Key Words: GIT1 • VEGF • PLC ${gamma}$ • podosomes • endothelial cells