Endothelial epsins as regulators and potential therapeutic targets of tumor angiogenesis

被引:0
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作者
Kai Song
Hao Wu
H. N. Ashiqur Rahman
Yunzhou Dong
Aiyun Wen
Megan L. Brophy
Scott Wong
Sukyoung Kwak
Diane R. Bielenberg
Hong Chen
机构
[1] Harvard Medical School,Vascular Biology Program, Karp Family Research Laboratory, Department of Surgery, Boston Children’s Hospital
来源
关键词
Tumor angiogenesis; Endocytosis; VEGFR2; Signaling; Epsins; Target;
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摘要
VEGF-driven tumor angiogenesis has been validated as a central target in several tumor types deserving of continuous and further considerations to improve the efficacy and selectivity of the current therapeutic paradigms. Epsins, a family of endocytic clathrin adaptors, have been implicated in regulating endothelial cell VEGFR2 signaling, where its inactivation leads to nonproductive leaky neo-angiogenesis and, therefore, impedes tumor development and progression. Targeting endothelial epsins is of special significance due to its lack of affecting other angiogenic-signaling pathways or disrupting normal quiescent vessels, suggesting a selective modulation of tumor angiogenesis. This review highlights seminal findings on the critical role of endothelial epsins in tumor angiogenesis and their underlying molecular events, as well as strategies to prohibit the normal function of endogenous endothelial epsins that capitalize on these newly understood mechanisms.
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页码:393 / 398
页数:5
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