Vascular RhoJ is an effective and selective target for tumor angiogenesis and vascular disruption.

Journal: Cancer Cell
Published:
Abstract

Current antiangiogenic therapy is limited by its cytostatic nature and systemic side effects. To address these limitations, we have unveiled the role of RhoJ, an endothelial-enriched Rho GTPase, during tumor progression. RhoJ blockade provides a double assault on tumor vessels by both inhibiting tumor angiogenesis and disrupting the preformed tumor vessels through the activation of the RhoA-ROCK (Rho kinase) signaling pathway in tumor endothelial cells, consequently resulting in a functional failure of tumor vasculatures. Moreover, enhanced anticancer effects were observed when RhoJ blockade was employed in concert with a cytotoxic chemotherapeutic agent, angiogenesis-inhibiting agent, or vascular-disrupting agent. These results identify RhoJ blockade as a selective and effective therapeutic strategy for targeting tumor vasculature with minimal side effects.

Authors
Chan Kim, Hanseul Yang, Yoko Fukushima, Phei Saw, Junyeop Lee, Jin-sung Park, Intae Park, Jinmyung Jung, Hiroshi Kataoka, Doheon Lee, Won Heo, Injune Kim, Sangyong Jon, Ralf Adams, Shin-ichi Nishikawa, Akiyoshi Uemura, Gou Koh

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