Targeting pericyte-endothelial cell crosstalk by circular RNA-cPWWP2A inhibition aggravates diabetes-induced microvascular dysfunction

通过环状 RNA-cPWWP2A 抑制来靶向周细胞-内皮细胞串扰会加重糖尿病引起的微血管功能障碍

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作者：Chang Liu, Hui-Min Ge, Bai-Hui Liu, Rui Dong, Kun Shan, Xue Chen, Mu-Di Yao, Xiu-Miao Li, Jin Yao, Rong-Mei Zhou, Shu-Jie Zhang, Qin Jiang, Chen Zhao, Biao Yan

期刊：	Proceedings of the National Academy of Sciences of the United States of America	影响因子：
时间：	2019	起止号：	2019 Apr 9;116(15):7455-7464.
doi：	10.1073/pnas.1814874116	研究方向：	代谢
疾病类型：	糖尿病	细胞类型：	内皮细胞

Abstract

The crosstalk between vascular pericytes and endothelial cells (ECs) is critical for microvascular stabilization and remodeling; however, the crosstalk is often disrupted by diabetes, leading to severe and even lethal vascular damage. Circular RNAs are a class of endogenous RNAs that regulate several important physiological and pathological processes. Here we show that diabetes-related stress up-regulates cPWWP2A expression in pericytes but not in ECs. In vitro studies show that cPWWP2A directly regulates pericyte biology but indirectly regulates EC biology via exosomes carrying cPWWP2A. cPWWP2A acts as an endogenous miR-579 sponge to sequester and inhibit miR-579 activity, leading to increased expression of angiopoietin 1, occludin, and SIRT1. In vivo studies show that cPWWP2A overexpression or miR-579 inhibition alleviates diabetes mellitus-induced retinal vascular dysfunction. By contrast, inhibition of cPWWP2A-mediated signaling by silencing cPWWP2A or overexpressing miR-579 aggravates retinal vascular dysfunction. Collectively, this study unveils a mechanism by which pericytes and ECs communicate. Intervention of cPWWP2A or miR-579 expression may offer opportunities for treating diabetic microvascular complications.

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