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首页> 外文期刊>Seminars in immunopathology >Aryl hydrocarbon receptor promotes RORγt+ Group 3 ILCs and controls intestinal immunity and inflammation
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Aryl hydrocarbon receptor promotes RORγt+ Group 3 ILCs and controls intestinal immunity and inflammation

机译:芳烃受体可促进RORγt+ 3类ILC并控制肠道免疫力和炎症

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Unlike adaptive immune cells that require antigen recognition and functional maturation during infection, innate lymphoid cells (ILCs) usually respond to pathogens promptly and serve as the first line of defense in infectious diseases. RAR-related orphan receptor (RORγt)+ group 3 ILCs are one of the innate cell populations that have recently been intensively studied. During the fetal stage of development, RORγt + group 3 ILCs (e.g., lymphoid tissue inducer cells) are required for lymphoid organogenesis. In adult mice, RORγt+ group 3 ILCs are abundantly present in the gut to exert immune defensive functions. Under certain circumstances, however, RORγt+ group 3 ILCs can be pathogenic and contribute to intestinal inflammation. Aryl hydrocarbon receptor (Ahr), a ligand-dependent transcriptional factor, is widely expressed by various immune and non-immune cells. In the gut, the ligand for Ahr can be derived/generated from diet, microflora, and/or host cells. Ahr has been shown to regulate different cell populations in the immune system including RORγt+ group 3 ILCs, T helper (Th)17/22 cells, γδT cells, regulatory T cells (Tregs), Tr1 cells, and antigen presenting cells. In this review, we will focus on the development and function of RORγt + group 3 ILCs, and discuss the role of Ahr in intestinal immunity and inflammation in mice and in humans. A better understanding of the function of Ahr in the gut is important for developing new therapeutic means to target Ahr in future treatment of infectious and autoimmune diseases.
机译:与在感染过程中需要抗原识别和功能成熟的适应性免疫细胞不同,先天性淋巴样细胞(ILC)通常对病原体迅速做出反应,并成为传染病的第一道防线。 RAR相关的孤儿受体(RORγt)+第3组ILC是最近被广泛研究的先天细胞群体之一。在胎儿发育阶段,淋巴器官发生需要RORγt+第3组ILC(例如淋巴组织诱导细胞)。在成年小鼠中,肠道中大量存在RORγt+ 3类ILC,以发挥免疫防御功能。但是,在某些情况下,RORγt+ 3类ILC可能是致病性的,并引起肠道炎症。芳烃受体(Ahr)是一种依赖配体的转录因子,被各种免疫和非免疫细胞广泛表达。在肠道中,Ahr的配体可以从饮食,微生物区系和/或宿主细胞衍生/产生。已显示Ahr可调节免疫系统中的不同细胞群,包括RORγt+ 3组ILC,T辅助(Th)17/22细胞,γδT细胞,调节性T细胞(Tregs),Tr1细胞和抗原呈递细胞。在这篇综述中,我们将专注于RORγt+第3组ILC的发展和功能,并讨论Ahr在小鼠和人类肠道免疫和炎症中的作用。更好地了解Ahr在肠道中的功能对于开发靶向Ahr的新治疗手段非常重要,可用于将来治疗传染性和自身免疫性疾病。

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