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Essential Roles of CD8+CD122+ Regulatory T Cells in the Maintenance of T Cell Homeostasis

机译:CD8 + CD122 +调节性T细胞在维持T细胞稳态中的重要作用

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摘要

Regulation of immune system is of paramount importance to prevent immune attacks against self-components. Mice deficient in the interleukin (IL)-2/IL-15 receptor β chain, CD122, are model animals of such immune attacks and characteristically have a high number of abnormally activated T cells. Here, we show that the transfer of CD8+CD122+ cells into CD122-deficient neonates totally prevented the development of abnormal T cells. Furthermore, recombination activating gene–2−/− mice that received wild-type mice–derived CD8+CD122− cells died within 10 wk after cell transfer, indicating that normal CD8+CD122− cells become dangerously activated T cells in the absence of CD8+CD122+ T cells. CD8+CD122+ cells could control activated CD8+ or CD4+ T cells both in vivo and in vitro. Our results indicate that the CD8+CD122+ population includes naturally occurring CD8+ regulatory T cells that control potentially dangerous T cells.
机译:免疫系统的调节对于防止针对自身成分的免疫攻击至关重要。白细胞介素(IL)-2 / IL-15受体β链CD122缺陷的小鼠是这种免疫攻击的模型动物,其特征是具有大量异常激活的T细胞。在这里,我们表明,将CD8 + CD122 +细胞转移到CD122缺陷型新生儿中完全可以阻止异常T细胞的发育。此外,接受野生型小鼠衍生的CD8 + CD122-细胞的重组激活基因2-/-小鼠在细胞转移后10 wk内死亡,这表明正常的CD8 + CD122-细胞在没有CD8的情况下变成危险激活的T细胞。 + CD122 + T细胞。 CD8 + CD122 +细胞可以在体内和体外控制活化的CD8 +或CD4 + T细胞。我们的结果表明,CD8 + CD122 +群体包括控制潜在危险T细胞的天然CD8 +调节性T细胞。

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