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Th17 cells in immunity and autoimmunity.

机译:Th17细胞具有免疫和自身免疫功能。

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The primary function of Th17 cells appears to be the clearance of extracellular pathogens during infections. However, Th17 cells also promote inflammation and have been implicated in the pathogenesis of many experimental autoimmune diseases and human inflammatory conditions. Transforming growth factor beta (TGFbeta) is a critical differentiation factor for the generation of regulatory T (T-reg) cells, whereas the combination of interleukin 6 (IL6) and TGFbeta induces the differentiation of pathogenic Th17 cells. Therefore, it is proposed that at the steady state (in the absence of any inflammatory stimuli), TGFbeta, which is produced by various cells types including naturally occurring T-reg (nT-reg) cells, encourages the generation of induced T-reg (iT-reg) cells, which together with nT-reg cells keep autoreactive T cells under check. IL6, an acute phase protein produced by the activated immune system, inhibits the function of T-reg cells and instead promotes the differentiation of Th17 cells. Thus, IL6 plays a pivotal role in dictating the balance between the generation of T-reg and Th17 cells. This reciprocal relationship between T-reg and Th17 cells is further supported by the results obtained in IL6(-/-) mice, which show a severe defect in the generation of Th17 cells and increased numbers of T-reg cells in the peripheral repertoire.
机译:Th17细胞的主要功能似乎是感染期间清除细胞外病原体。但是,Th17细胞也促进炎症,并与许多实验性自身免疫性疾病和人类炎症性疾病的发病机理有关。转化生长因子β(TGFbeta)是调节性T(T-reg)细胞生成的关键分化因子,而白介素6(IL6)和TGFbeta的组合可诱导致病性Th17细胞分化。因此,有人提出,在稳态下(在没有任何炎症刺激的情况下),由包括天然存在的T-reg(nT-reg)细胞在内的各种细胞类型产生的TGFbeta会促进诱导型T-reg的产生。 (iT-reg)细胞与nT-reg细胞一起使自身反应性T细胞受到检查。 IL6是一种由活化的免疫系统产生的急性期蛋白,可抑制T-reg细胞的功能,并促进Th17细胞的分化。因此,IL6在决定T-reg和Th17细胞生成之间的平衡中起关键作用。在IL6(-/-)小鼠中获得的结果进一步支持了T-reg和Th17细胞之间的这种相互关系,该结果显示Th17细胞的生成存在严重缺陷,并且外周血T-reg细胞数量增加。

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