| Literature DB >> 28612217 |
Bing Liu1,2,3, Hengchi Yu1,2,3, Guangyong Sun2,3,4, Xiaojing Sun2,3,4, Hua Jin2,3,4, Chunpan Zhang2,3,4, Wen Shi2,3,4, Dan Tian2,3,4, Kai Liu2,3,4, Hufeng Xu2,3,4, Xinmin Li2,3,4, Jie Yin1, Xu Hong5, Dong Zhang6,7,8.
Abstract
Adaptive immunity plays a critical role in IR and T2DM development; however, the biological mechanisms linking T cell costimulation and glucose metabolism have not been fully elucidated. In this study, we demonstrated that the costimulatory molecule OX40 controls T cell activation and IR development. Inflammatory cell accumulation and enhanced proinflammatory gene expression, as well as high OX40 expression levels on CD4+ T cells, were observed in the adipose tissues of mice with diet-induced obesity. OX40-KO mice exhibited significantly less weight gain and lower fasting glucose levels than those of WT mice, without obvious adipose tissue inflammation. The effects of OX40 on IR are mechanistically linked to the promotion of T cell activation, Th1 cell differentiation and proliferation-as well as the attenuation of Treg suppressive activity and the enhancement of proinflammatory cytokine production-in adipose tissues. Furthermore, OX40 expression on T cells was positively associated with obesity in humans, suggesting that our findings are clinically relevant. In summary, our study revealed that OX40 in CD4+ T cells is crucial for adipose tissue inflammation and IR development. Therefore, the OX40 signaling pathway may be a new target for preventing or treating obesity-related IR and T2DM.Entities:
Keywords: Adipocyte; Adipose inflammation; Costimulation molecule; Diet-induced obesity; High-fat diet; IFN-γ; IL-17a; Immunology; Regulatory T cells; Th1; Th17
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Year: 2017 PMID: 28612217 DOI: 10.1007/s00018-017-2552-7
Source DB: PubMed Journal: Cell Mol Life Sci ISSN: 1420-682X Impact factor: 9.261