首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Innate signals compensate for the absence of PKC-theta during in vivo CD8+T cell effector and memory responses
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Innate signals compensate for the absence of PKC-theta during in vivo CD8+T cell effector and memory responses

机译:先天性信号补偿体内CD8 + T细胞效应子和记忆反应过程中PKC-theta的缺失

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摘要

PKC-theta is central to T-helper (Th) 2 cell differentiation and effector function; however, its importance for antiviral effector, and in particular memory CD8+ T cell responses, remains unclear. We have investigated the role of PKC-theta during in vivo and in vitro responses against influenza virus, lymphocytic choriomeningitis virus, vaccinia virus, and replication-deficient virus-like particles. In the absence of PKC-theta, antiviral CD8+ T cells presented an unresponsive phenotype in vitro, which could be restored with exogenous IL-2 or by Toll-like receptor ligand-activated dendritic cells. In striking contrast, PKC-theta appeared to be superfluous for in vivo antiviral responses irrespective of whether the virus infected systemically, was localized to the lung, or did not replicate. In addition, CD8+ CCR7-effector memory responses were normal in PKC-theta-deficient mice, both in lymphoid and peripheral tissues. Our data show that increased activation signals delivered in vivo by highly activated dendritic cells, as present during viral infections, overcome the requirement for PKC-theta during CD8+ T cell antiviral responses.
机译:PKC-θ是T-helper(Th)2细胞分化和效应子功能的关键;然而,其对于抗病毒效应物,特别是记忆CD8 + T细胞应答的重要性尚不清楚。我们已经研究了PKC-theta在针对流感病毒,淋巴细胞性脉络膜脑膜炎病毒,牛痘病毒和复制缺陷型病毒样颗粒的体内和体外反应中的作用。在没有PKC-θ的情况下,抗病毒CD8 + T细胞在体外表现出无反应的表型,可以用外源IL-2或通过Toll样受体配体激活的树突状细胞恢复。与之形成鲜明对比的是,PKC-theta似乎对于体内抗病毒反应是多余的,无论该病毒是全身感染,位于肺部还是未复制。另外,在PKC-θ缺陷型小鼠的淋巴和周围组织中,CD8 + CCR7效应记忆反应是正常的。我们的数据表明,病毒感染期间存在的高活化树突状细胞在体内传递的活化信号增加,克服了CD8 + T细胞抗病毒反应期间PKC-theta的要求。

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