Advanced glycation end products induce immature angiogenesis in in vivo and ex vivo mouse models

被引:39
作者
Chen, Lixian [1 ]
Cui, Yun [1 ]
Li, Bingyu [1 ]
Weng, Jie [1 ]
Wang, Weiju [1 ]
Zhang, Shuangshuang [1 ]
Huang, Xuliang [1 ]
Guo, Xiaohua [1 ]
Huang, Qiaobing [1 ]
机构
[1] Southern Med Univ, Sch Basic Med Sci, Dept Pathophysiol, Guangdong Prov Key Lab Shock & Microcirculat, Guangzhou, Peoples R China
来源
AMERICAN JOURNAL OF PHYSIOLOGY-HEART AND CIRCULATORY PHYSIOLOGY | 2020年 / 318卷 / 03期
基金
中国国家自然科学基金;
关键词
advanced glycation end products; moesin phosphorylation; pericyte; RAGE; RhoA/ROCK; EZRIN/RADIXIN/MOESIN PROTEINS; VASCULAR HYPERPERMEABILITY; RETINAL ANGIOGENESIS; DIABETIC-RETINOPATHY; MOLECULAR REGULATION; ENDOTHELIAL-CELLS; RAGE AXIS; RECEPTOR; MIGRATION; AGES;
D O I
10.1152/ajpheart.00473.2019
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Proliferative diabetic retinopathy (PDR) is a progressive disease predominantly involving pathological angiogenesis and is characterized by the development of immature, fragile, and easily hemorrhagic new vessels. Advanced glycation end products (AGEs) and the receptor for AGEs (RAGE) play important roles in the progression of diabetic retinopathy. Our previous studies demonstrated that AGEs promoted HUVEC angiogenesis by inducing moesin phosphorylation via RhoA/Rho-associated protein kinase (ROCK) pathway. The aim of this study was to further confirm AGE-induced angiogenesis in vivo and the involvement of RAGE. ROCK, and moesin phosphorylation in this process. We performed the study in an AGE-treated mouse model with various angiogenesis assays in multiple in vivo and ex vivo models. The results demonstrated that AGEs promoted significant neovascularization in whole mount retina and mouse aortic ring of adult and postnatal mice and in Matrigel plug as well, which were consistently accompanied by increased moesin phosphorylation. The increase of AGE-evoked neovascularization and moesin phosphorylation were both attenuated by RAGE knockout or ROCK inhibitor Y27632 administration in mice. We also revealed the pathological characteristics of AGE-promoted angiogenesis by demonstrating the decrease of pericyte coverage and the disarranged endothelial alignment in microvessels. In conclusion, this study provides in vivo evidences that AGEs induce immature angiogenesis by binding to RAGE, activating the RhoA/ROCK signal pathway and inducing moesin phosphorylation. NEW & NOTEWORTHY Advanced glycation end product (AGE)-induced formation of neovessels and phosphorylation of moesin in retina and aortic ring required AGE receptors. AGEs increased neovessels and the phosphorylation of moesin in retina and aortic ring via RhoA/ROCK pathway. AGE-induced immature angiogenesis in AGE-treated mouse retina and aortic ring. The AGE-RAGE axis and moesin could be candidate targets for overcoming relative diseases.
引用
收藏
页码:H519 / H533
页数:15
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