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Trans-presentation of IL-15 modulates STAT5 activation and Bcl-6 expression in TH1 cells

机译:IL-15的转染调节T H 1细胞中STAT5激活和Bcl-6表达

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During infection, na?ve CD4+ T helper cells differentiate into specialized effector subsets based upon environmental signals propagated by the cytokine milieu. Recently, this paradigm has been complicated by the demonstration that alterations in the cytokine environment can result in varying degrees of plasticity between effector T helper cell populations. Therefore, elucidation of the mechanisms by which cytokines regulate T helper cell differentiation decisions is increasingly important. The gamma common cytokine IL-15 is currently undergoing clinical trials for the treatment of malignancies, due to its well-established role in the regulation of natural killer and CD8+ T cell immune responses. However, the effect of IL-15 signaling on CD4+ T cell activity is incompletely understood. One mechanism by which IL-15 activity is conferred is through trans-presentation via the IL-15 receptor alpha subunit. Here, we demonstrate that differentiated TH1 cells are responsive to trans-presented IL-15. Importantly, while trans-presentation of IL-15 results in STAT5 activation and maintenance of the TH1 gene program, IL-15 treatment alone allows for increased Bcl-6 expression and the upregulation of a TFH-like profile. Collectively, these findings describe a novel role for IL-15 in the modulation of CD4+ T cell responses and provide valuable insight for the use of IL-15 in immunotherapeutic approaches.
机译:在感染过程中,幼稚的CD4 + T辅助细胞会根据细胞因子环境所传播的环境信号而分化成专门的效应子亚群。最近,由于细胞因子环境的改变可导致效应T辅助细胞群之间不同程度的可塑性的证明,使该范例变得复杂。因此,阐明细胞因子调节T辅助细胞分化决定的机制变得越来越重要。 γ共同细胞因子IL-15由于其在调节自然杀伤细胞和CD8 + T细胞免疫反应中的公认作用,目前正在临床治疗恶性肿瘤。但是,IL-15信号对CD4 + T细胞活性的影响尚不完全清楚。赋予IL-15活性的一种机制是通过IL-15受体α亚基进行转递。在这里,我们证明了分化的T H 1细胞对转染的IL-15有反应。重要的是,虽然IL-15的转座导致STAT5激活和T H 1基因程序的维持,但单独的IL-15治疗可以增加Bcl-6的表达并上调T < sub> FH 之类的配置文件。这些发现共同说明了IL-15在调节CD4 + T细胞应答中的新作用,并为IL-15在免疫治疗方法中的应用提供了有价值的见解。

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