Adipocyte-secreted exosomal microRNA-34a inhibits M2 macrophage polarization to promote obesity-induced adipose inflammation

脂肪组织 脂肪细胞 内分泌学 内科学 炎症 小RNA 脂肪组织巨噬细胞 巨噬细胞极化 肥胖 白色脂肪组织 生物 分泌物 细胞生物学 化学 医学 巨噬细胞 基因 生物化学 体外
作者
Yong Pan,Xiaoyan Hui,Ruby L.C. Hoo,Dewei Ye,Cyrus Yuk Cheung Chan,Tianshi Feng,Yu Wang,Karen Siu Ling Lam,Aimin Xu
出处
期刊:Journal of Clinical Investigation [American Society for Clinical Investigation]
卷期号:129 (2): 834-849 被引量:395
标识
DOI:10.1172/jci123069
摘要

Persistent, unresolved inflammation in adipose tissue is a major contributor to obesity-associated metabolic complications. However, the molecular links between lipid-overloaded adipocytes and inflammatory immune cells in obese adipose tissues remain elusive. Here we identified adipocyte-secreted microRNA-34a (miR-34a) as a key mediator through its paracrine actions on adipose-resident macrophages. The expression of miR-34a in adipose tissues was progressively increased with the development of dietary obesity. Adipose-selective or adipocyte-specific miR-34a-KO mice were resistant to obesity-induced glucose intolerance, insulin resistance, and systemic inflammation, and this was accompanied by a significant shift in polarization of adipose-resident macrophages from proinflammatory M1 to antiinflammatory M2 phenotype. Mechanistically, mature adipocyte-secreted exosomes transported miR-34a into macrophages, thereby suppressing M2 polarization by repressing the expression of Krüppel-like factor 4 (Klf4). The suppressive effects of miR-34a on M2 polarization and its stimulation of inflammatory responses were reversed by ectopic expression of Klf4 in both bone marrow-derived macrophages and adipose depots of obese mice. Furthermore, increased miR-34a expression in visceral fat of overweight/obese subjects correlated negatively with reduced Klf4 expression, but positively with the parameters of insulin resistance and metabolic inflammation. In summary, miR-34a was a key component of adipocyte-secreted exosomal vesicles that transmitted the signal of nutrient overload to the adipose-resident macrophages for exacerbation of obesity-induced systemic inflammation and metabolic dysregulation.
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