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Antigen-Independent IFN-γ Production by Human Naïve CD4+ T Cells Activated by IL-12 Plus IL-18

机译:IL-12 Plus IL-18激活的人幼稚CD4 + T细胞产生的抗原非依赖性IFN-γ产生

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摘要

The role of T cells in innate immunity is not well defined. In this report, we show that a subset of human peripheral blood CD4+ T cells responds to IL-12 plus IL-18, but not to IL-12 or IL-18 alone, by producing IFN-γ in the absence of any antigenic stimulation or cell proliferation. Intracellular staining reveals a small percentage of resting CD4+ T cells (0.5 to 1.5%) capable of producing IFN-γ in response to IL-12 plus IL-18. Interestingly, both naïve (CD45RA+) and memory (CD45RO+) CD4+ populations were responsive to IL-12 plus IL-18 stimulation in producing IFN-γ. The expression of IFN-γinduced by IL-12 and IL-18 is sensitive to rapamycin and SB203580, indicating the possible involvement of mTOR and p38 MAP kinase, respectively, in this synergistic pathway. While p38MAP kinase is involved in transcription, mTOR is involved in message stabilization. We have also shown that NFκB family member, cRel, but not GADD45β and GADD45γ, plays an important role in IL-12 plus IL-18-induced IFN-γ transcription. Thus, the present study suggests that naïve CD4+ T cells may participate in innate immunity or amplify adaptive immune responses through cytokine-induced antigen-independent cytokine production.
机译:T细胞在先天免疫中的作用尚不清楚。在这份报告中,我们显示了人类外周血CD4 + T细胞的一个子集通过产生IFN-γ对IL-12加IL-18做出反应,但对单独的IL-12或IL-18没有反应。 γ在没有任何抗原刺激或细胞增殖的情况下。细胞内染色显示,小部分的静息CD4 + T细胞(0.5%至1.5%)能够响应IL-12和IL-18产生IFN-γ。有趣的是,幼稚(CD45RA + )和记忆(CD45RO + )CD4 + 种群均对IL-12和IL-18刺激产生反应。产生IFN-γ。 IL-12和IL-18诱导的IFN-γ的表达对雷帕霉素和SB203580敏感,表明mTOR和p38 MAP激酶可能分别参与了这种协同途径。虽然p38MAP激酶参与转录,但mTOR参与消息稳定。我们还显示,NFκB家族成员cRel,而不是GADD45β和GADD45γ,在IL-12加IL-18诱导的IFN-γ转录中起重要作用。因此,本研究表明,幼稚的CD4 + T细胞可能通过细胞因子诱导的抗原非依赖性细胞因子的产生参与先天免疫或增强适应性免疫反应。

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