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首页> 外文期刊>The journal of immunology >Parallel Expansion of Human Virus-Specific FoxP3? Effector Memory and De Novo-Generated FoxP3+ Regulatory CD8+ T Cells upon Antigen Recognition In Vitro
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Parallel Expansion of Human Virus-Specific FoxP3? Effector Memory and De Novo-Generated FoxP3+ Regulatory CD8+ T Cells upon Antigen Recognition In Vitro

机译:并行扩展特定于人类病毒的FoxP3?抗原识别后的效应记忆和从头产生的FoxP3 +调节性CD8 + T细胞

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Although FoxP3 has been shown to be the most specific marker for regulatory CD4+ T cells, its significance in the CD8+ T cell population is not well understood. In this study, we show that the in vitro stimulation of human PBMC with hepatitis C virus or Flu virus-specific peptides gives rise to two distinct Ag-specific T cell populations: FoxP3? and FoxP3+CD8+ T cells. The FoxP3+ virus-specific CD8+ T cells share phenotypical markers of regulatory T cells, such as CTLA-4 and glucocorticoid-induced TNFR family-related gene, and do produce moderate amounts of IFN-γ but not IL-2 or IL-10. IL-2 and IL-10 are critical cytokines, however, because the expansion of virus-specific FoxP3+CD8+ T cells is blocked by IL-2- or IL-10-neutralizing mAbs. The virus-specific FoxP3+CD8+ T cells have a reduced proliferative capacity, indicating anergy, and display a cell-cell contact-dependent suppressive activity. Taken together, our results indicate that stimulation with a defined viral Ag leads to the expansion of two different cell populations: FoxP3? memory/effector as well as FoxP3+ regulatory virus-specific CD8+ T cells.
机译:尽管已显示FoxP3是调节性CD4 + T细胞的最特异标志物,但其在CD8 + T细胞群体中的重要性尚不清楚。在这项研究中,我们表明用丙型肝炎病毒或流感病毒特异性肽体外刺激人PBMC会产生两个不同的Ag特异性T细胞群体:FoxP3?和FoxP3 + CD8 + T细胞。 FoxP3 +病毒特异性CD8 + T细胞共享调节性T细胞的表型标记,例如CTLA-4和糖皮质激素诱导的TNFR家族相关基因,并且确实产生中等量的IFN-γ,但不产生IL-2或IL-10。但是,IL-2和IL-10是关键的细胞因子,因为病毒特异性FoxP3 + CD8 + T细胞的扩增被IL-2-或IL-10-中和mAb阻断。病毒特异性FoxP3 + CD8 + T细胞的增殖能力降低,表明无反应,并表现出细胞-细胞接触依赖性抑制活性。两者合计,我们的结果表明,用确定的病毒Ag刺激会导致两个不同细胞群的扩增:FoxP3?记忆/效应子以及FoxP3 +调节性病毒特异性CD8 + T细胞。

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