Brown adipose tissue-derived Nrg4 alleviates endothelial inflammation and atherosclerosis in male mice
Shi Lingfeng, Li Yixiang, Xu Xiaoli, Cheng Yangyang, Meng Biying, Xu Jinling, Xiang Lin, Zhang Jiajia, He Kaiyue, Tong Jiayue, Zhang Junxia, Xiang Lingwei, Xiang Guangda
Journal:Nature Metabolism
IF:19.87
DOI:10.1038/s42255-022-00671-0
PMID:36400933
Published:2022-11-18
research field:分子生物学内分泌学心血管生物学
Abstract
Brown adipose tissue (BAT) activity contributes to cardiovascular health by its energy-dissipating capacity but how BAT modulates vascular function and atherosclerosis through endocrine mechanisms remains poorly understood. Here we show that BAT-derived neuregulin-4 (Nrg4) ameliorates atherosclerosis in mice. BAT-specific Nrg4 deficiency accelerates vascular inflammation and adhesion responses, endothelial dysfunction and apoptosis and atherosclerosis in male mice. BAT-specific Nrg4 restoration alleviates vascular inflammation and adhesion responses, attenuates leukocyte homing and reduces endothelial injury and atherosclerosis in male mice. In endothelial cells, Nrg4 decreases apoptosis, inflammation and adhesion responses induced by oxidized low-density lipoprotein. Mechanistically, protein kinase B (Akt)–nuclear factor-κB signaling is involved in the beneficial effects of Nrg4 on the endothelium. Taken together, the results reveal Nrg4 as a potential cross-talk factor between BAT and arteries that may serve as a target for atherosclerosis.
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