| Literature DB >> 30380415 |
Huan Zhao1, Xueying Tian2, Lingjuan He1, Yan Li1, Wenjuan Pu1, Qiaozhen Liu1, Juan Tang1, Jiaying Wu3, Xin Cheng3, Yang Liu4, Qingtong Zhou5, Zhen Tan6, Fan Bai4, Fei Xu7, Nicola Smart8, Bin Zhou9.
Abstract
Identification of cellular surface markers that distinguish tumorous from normal vasculature is important for the development of tumor vessel-targeted therapy. Here, we show that Apj, a G protein-coupled receptor, is highly enriched in tumor endothelial cells but absent from most endothelial cells of adult tissues in homeostasis. By genetic targeting using Apj-CreER and Apj-DTRGFP-Luciferase, we demonstrated that hypoxia-VEGF signaling drives expansion of Apj+ tumor vessels and that targeting of these vessels, genetically and pharmacologically, remarkably inhibits tumor angiogenesis and restricts tumor growth. These in vivo findings implicate Apj+ vessels as a key driver of pathological angiogenesis and identify Apj+ endothelial cells as an important therapeutic target for the anti-angiogenic treatment of tumors.Entities:
Keywords: Angiogenesis; Apj; anti-angiogenic treatment; surface marker; tumor therapeutic target; tumorous vessel
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Year: 2018 PMID: 30380415 DOI: 10.1016/j.celrep.2018.10.015
Source DB: PubMed Journal: Cell Rep Impact factor: 9.995