Plexin-B1 activates NF-κB and IL-8 to promote a pro-angiogenic response in endothelial cells.

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RESEARCH PRODUCT

Plexin-B1 activates NF-κB and IL-8 to promote a pro-angiogenic response in endothelial cells.

Patrizia Proia Patrizia Proia Hua Zhou Ying-hua Yang John R. Basile John R. Basile Nada O. Binmadi

subject

animal structures RHOA Proto-Oncogene Proteins c-akt Angiogenesis Signaling in cellular processes G-protein signaling Cancer Treatment SEMA4D lcsh:Medicine Signal transduction Biology 03 medical and health sciences Molecular cell biology 0302 clinical medicine Semaphorin Settore BIO/10 - Biochimica Akt Signaling Cascade Membrane Receptor Signaling Interleukin 8 lcsh:Science Biology Protein kinase B GTPase signaling Ras signaling 030304 developmental biology 0303 health sciences Multidisciplinary Mechanisms of Signal Transduction lcsh:R Signaling Cascades 3. Good health Cell biology Plexin B1 RNA interference pro-angiogenic endothelial cells Oncology 030220 oncology & carcinogenesis embryonic structures Cancer research biology.protein Medicine lcsh:Q Antiangiogenesis Therapy Antiapoptotic signaling Signal transduction Research Article

description

Background The semaphorins and their receptors, the plexins, are proteins related to c-Met and the scatter factors that have been implicated in an expanding signal transduction network involving co-receptors, RhoA and Ras activation and deactivation, and phosphorylation events. Our previous work has demonstrated that Semaphorin 4D (Sema4D) acts through its receptor, Plexin-B1, on endothelial cells to promote angiogenesis in a RhoA and Akt-dependent manner. Since NF-κB has been linked to promotion of angiogenesis and can be activated by Akt in some contexts, we wanted to examine NF-κB in Sema4D treated cells to determine if there was biological significance for the pro-angiogenic phenotype observed in endothelium. Methods/Principal Findings Using RNA interference techniques, gel shifts and NF-κB reporter assays, we demonstrated NF-κB translocation to the nucleus in Sema4D treated endothelial cells occurring downstream of Plexin-B1. This response was necessary for endothelial cell migration and capillary tube formation and protected endothelial cells against apoptosis as well, but had no effect on cell proliferation. We dissected Plexin-B1 signaling with chimeric receptor constructs and discovered that the ability to activate NF-κB was dependent upon Plexin-B1 acting through Rho and Akt, but did not involve its role as a Ras inhibitor. Indeed, inhibition of Rho by C3 toxin and Akt by LY294002 blocked Sema4D-mediated endothelial cell migration and tubulogenesis. We also observed that Sema4D treatment of endothelial cells induced production of the NF-κB downstream target IL-8, a response necessary for angiogenesis. Finally, we could show through co-immunofluorescence for p65 and CD31 that Sema4D produced by tumor xenografts in nude mice activated NF-κB in vessels of the tumor stroma. Conclusion/Significance These findings provide evidence that Sema4D/Plexin-B1-mediated NF-κB activation and IL-8 production is critical in the generation a pro-angiogenic phenotype in endothelial cells and suggests a new therapeutic target for the anti-angiogenic treatment of some cancers.

year	journal	country	edition	language
2011-10-18	PLoS ONE

10.1371/journal.pone.0025826 http://europepmc.org/articles/PMC3196529?pdf=render