Targeting Nuclear Receptors for TH17-Mediated Inflammation: REV-ERBerations of Circadian Rhythm and Metabolism.

Sarah A Mosure, Adrianna N Wilson, Laura A Solt
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引用次数: 2

Abstract

Since their discovery, a significant amount of progress has been made understanding T helper 17 (TH17) cells' roles in immune homeostasis and disease. Outside of classical cytokine signaling, environmental and cellular intrinsic factors, including metabolism, have proven to be critical for non-pathogenic vs pathogenic TH17 cell development, clearance of infections, and disease. The nuclear receptor RORγt has been identified as a key regulator of TH17-mediated inflammation. Nuclear receptors regulate a variety of physiological processes, ranging from reproduction to the circadian rhythm, immunity to metabolism. Outside of RORγt, the roles of other nuclear receptors in TH17-mediated immunity are not as well established. In this mini-review we describe recent studies that revealed a role for a different member of the nuclear receptor superfamily, REV-ERBα, in the regulation of TH17 cells and autoimmunity. We highlight similarities and differences between reports, potential roles beyond TH17-mediated cytokine regulation, unresolved questions in the field, as well as the translational potential of targeting REV-ERBα.

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靶向th17介导炎症的核受体:昼夜节律和代谢的rev - erations。
自发现以来,人们对辅助性T - 17 (TH17)细胞在免疫稳态和疾病中的作用的理解取得了重大进展。除了经典的细胞因子信号外,环境和细胞内在因素,包括代谢,已被证明对非致病性和致病性TH17细胞发育、感染清除和疾病至关重要。核受体RORγt已被确定为th17介导的炎症的关键调节因子。核受体调节多种生理过程,从生殖到昼夜节律,从免疫到代谢。除RORγt外,其他核受体在th17介导的免疫中的作用尚未确定。在这篇小型综述中,我们描述了最近的研究,揭示了核受体超家族的不同成员rev - erba在TH17细胞和自身免疫调节中的作用。我们强调了报告之间的异同,th17介导的细胞因子调控之外的潜在作用,该领域未解决的问题,以及靶向rev - erba的翻译潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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