干扰素调节因子 3 控制 CD8 T 淋巴细胞中白细胞介素-17 的表达。
Interferon regulatory factor 3 controls interleukin-17 expression in CD8 T lymphocytes.
机构信息
Institute for Medical Immunology, Walloon Excellence in Life sciences and BIOtechnology, Université Libre de Bruxelles, B-6041 Charleroi-Gosselies, Belgium.
出版信息
Proc Natl Acad Sci U S A. 2013 Aug 20;110(34):E3189-97. doi: 10.1073/pnas.1219221110. Epub 2013 Aug 5.
Abstract
IFN regulatory factor (IRF) 3 plays a key role in innate responses against viruses. Herein we assessed its contribution to T-cell activation. We observed that poly(I:C)-induced IRF3 activation in CD8 T cells represses IL-17 expression in a type I IFN-independent fashion. Even in the absence of poly(I:C), polyclonally activated naïve IRF3(-/-) CD8 T cells expressed high levels of IL-17 and IL-23R in comparison with wild-type cells. Furthermore, IRF3(-/-) OT1 cells adoptively transferred into wild-type hosts also produced higher IL-17 levels upon immunization than their wild-type counterparts. This phenotype could be reversed by ectopic expression of IRF3, confirming that this effect is intrinsic to T cells. We show that IRF3 directly interacts with RORγt in the cytoplasm through its IRF interaction domain and limits its ability to bind and transactivate the IL-17 promoter. These observations uncover an unexpected role of IRF3 in the control of CD8 T-cell polarization.
摘要
干扰素调节因子(IRF)3 在抗病毒的先天免疫反应中起着关键作用。在此,我们评估了它对 T 细胞激活的贡献。我们观察到聚(I:C)诱导的 CD8 T 细胞中的 IRF3 激活以一种不依赖 I 型干扰素的方式抑制了 IL-17 的表达。即使不存在聚(I:C),多克隆激活的幼稚 IRF3(-/-) CD8 T 细胞也比野生型细胞表达更高水平的 IL-17 和 IL-23R。此外,IRF3(-/-) OT1 细胞过继转移到野生型宿主中,在免疫后也比其野生型细胞产生更高水平的 IL-17。这种表型可以通过 IRF3 的异位表达逆转,证实了这种效应是 T 细胞固有的。我们表明,IRF3 通过其 IRF 相互作用结构域在细胞质中与 RORγt 直接相互作用,并限制其结合和转录激活 IL-17 启动子的能力。这些观察结果揭示了 IRF3 在控制 CD8 T 细胞极化中的意外作用。
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