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Nsun2 coupling with RoRγt shapes the fate of Th17 cells and promotes colitis.

Wen-Lan YangWeinan QiuTing ZhangKai XuZi-Juan GuYu ZhouHeng-Ji XuZhong-Zhou YangBin ShenYong-Liang ZhaoQi ZhouYing YangWei LiPeng-Yuan YangYun-Gui Yang
Published in: Nature communications (2023)
T helper 17 (Th17) cells are a subset of CD4 + T helper cells involved in the inflammatory response in autoimmunity. Th17 cells secrete Th17 specific cytokines, such as IL-17A and IL17-F, which are governed by the master transcription factor RoRγt. However, the epigenetic mechanism regulating Th17 cell function is still not fully understood. Here, we reveal that deletion of RNA 5-methylcytosine (m 5 C) methyltransferase Nsun2 in mouse CD4 + T cells specifically inhibits Th17 cell differentiation and alleviates Th17 cell-induced colitis pathogenesis. Mechanistically, RoRγt can recruit Nsun2 to chromatin regions of their targets, including Il17a and Il17f, leading to the transcription-coupled m 5 C formation and consequently enhanced mRNA stability. Our study demonstrates a m 5 C mediated cell intrinsic function in Th17 cells and suggests Nsun2 as a potential therapeutic target for autoimmune disease.
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