BAT-derived miR-378a-3p facilitates endothelial angiogenic function and promotes wound healing

伤口愈合 功能(生物学) 血管生成 化学 癌症研究 细胞生物学 内皮 炎症 内皮干细胞 新生血管 医学
作者
Hongyan Deng,Yuyu Xie,Jiadai Liu,Jing Ge,Qianqian Kang,Rui He,Zhihan Wang,Xuemin Peng,Zengzhe Zhu,Wenshe Wang,Yulian Liu,Ronghui Gao,Ruping Pan,Min Yang,Yong Chen
出处
期刊:JCI insight [American Society for Clinical Investigation]
标识
DOI:10.1172/jci.insight.201311
摘要

Interscapular brown adipose tissue (iBAT), one of the most vascularized tissues in the body, exemplifies the intricate crosstalk between the vascular system and adipocytes. BAT is known to secrete abundant exosomes into circulation, while exosomes are known to play a key role in vascular remodeling and cell migration. However, whether BAT-derived exosomes (BATexos) modulate peripheral vasculature remains unclear. Here, we report that BATexos promoted peripheral angiogenesis and vascular repair. Among their cargo, miR-378a-3p was highly enriched and identified as a key mediator of endothelial angiogenic function. The overexpression of miR-378a-3p in endothelial cells substantially promoted cell migration and tube formation. Conversely, inhibition of exosome secretion from BAT impaired vascular repair and delayed wound healing. Mechanistically, miR-378a-3p directly targeted the phosphatase and tensin homolog (Pten), thereby activating the PI3K-AKT signaling pathway. Liposomes encapsulating miR-378 mimics promoted angiogenesis and accelerated wound healing in a diabetic mouse model. Collectively, this study uncovers BAT-derived miR-378a-3p as a key regulator of vessel regeneration and tissue repair following injury, offering new therapeutic potential for treating vascular complications in metabolic disease.
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