| Literature DB >> 34330814 |
Yuli Lin1, Liuling Xiao2,3, Qian Cai1, Cuisong Zhu2, Shufen Li2, Bingji Li1, Ting Liu1, Qiongyue Zhang4, Yi Wang4, Yiming Li4, Xing He5, Dongning Pan2, Qiqun Tang2, Xiaohui Wu6, Weiqing Pan5, Jiqiu Wang7, Xi Li8, Rui He9,10.
Abstract
IL-33-associated type 2 innate immunity has been shown to support beige fat formation and thermogenesis in subcutaneous inguinal white adipose tissue (iWAT), but little is known about how it is regulated in iWAT. Chemerin, as a newly identified adipokine, is clinically associated with obesity and metabolic disorders. We here show that cold exposure specifically reduces chemerin and its receptor chemerin chemokine-like receptor 1 (CMKLR1) expression in iWAT. Lack of chemerin or adipocytic CMKLR1 enhances cold-induced thermogenic beige fat via potentiating type 2 innate immune responses. Mechanistically, we identify adipocytes, particularly beige adipocytes, as the main source for cold-induced IL-33, which is restricted by the chemerin-CMKLR1 axis via dampening cAMP-PKA signaling, thereby interrupting a feed-forward circuit between beige adipocytes and type 2 innate immunity that is required for cold-induced beige fat and thermogenesis. Moreover, specific deletion of adipocytic IL-33 inhibits cold-induced beige fat and type 2 innate immune responses. Last, genetic blockade of adipocytic CMKLR1 protects against diet-induced obesity and enhances the metabolic benefits of cold stimulation in preestablished obese mice. Thus, our study identifies the chemerin-CMKLR1 axis as a physiological negative regulator of thermogenic beige fat via interrupting adipose-immune communication and suggests targeting adipose CMKLR1 as a potential therapeutic strategy for obesity-related metabolic disorders.Entities:
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Year: 2021 PMID: 34330814 DOI: 10.1126/sciimmunol.abg9698
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468