首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Rapamycin-mediated enrichment of T cells with regulatory activity in stimulated CD4+ T cell cultures is not due to the selective expansion of naturally occurring regulatory T cells but to the induction of regulatory functions in conventional CD4+ T c
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Rapamycin-mediated enrichment of T cells with regulatory activity in stimulated CD4+ T cell cultures is not due to the selective expansion of naturally occurring regulatory T cells but to the induction of regulatory functions in conventional CD4+ T c

机译:雷帕霉素介导的T细胞在刺激的CD4 + T细胞培养物中具有调节活性的富集不是由于天然存在的调节T细胞的选择性扩增,而是由于诱导了常规CD4 + T c中的调节功能

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摘要

Rapamycin is an immunosuppressive drug currently used in different clinical settings. Although the capacity of rapamycin to inhibit the mammalian target of rapamycin serine/threonine protein kinase and therefore T cell cycle progression is well known, its effects are complex and not completely understood. It has been reported recently that TCR-mediated stimulation of murine CD4+ T cells in the presence of rapamycin results in increased proportions of CD4+ T cells with suppressive functions, suggesting that the drug may also exert its immunosuppressive activity by promoting the selective expansion of naturally occurring CD4+ regulatory T cells (Treg). In this study, we show that stimulation of human circulating CD4+ T cells in the presence of rapamycin results indeed in highly increased suppressor activity. By assessing the effect of rapamycin on the growth of nonregulatory and Treg populations of defined differentiation stages purified ex vivo from circulating CD4+ T cells, we could demonstrate that this phenomenon is not due to a selective expansion of naturally occurring Tregs, but to the capacity of rapamycin to induce, upon TCR-mediated stimulation, suppressor functions in conventional CD4+ T cells. This condition, however, is temporary and reversible as it is dependent upon the continuous presence of rapamycin.
机译:雷帕霉素是目前在不同临床环境中使用的一种免疫抑制药物。尽管雷帕霉素抑制雷帕霉素丝氨酸/苏氨酸蛋白激酶的哺乳动物靶标并因此抑制T细胞周期进程的能力是众所周知的,但是其作用是复杂的并且尚未完全被理解。最近有报道说,在雷帕霉素存在下,TCR介导的对鼠CD4 + T细胞的刺激导致具有抑制功能的CD4 + T细胞比例增加,这表明该药物还可以通过促进天然存在的选择性扩增来发挥其免疫抑制活性。 CD4 +调节性T细胞(Treg)。在这项研究中,我们表明在雷帕霉素的存在下刺激人循环CD4 + T细胞确实导致抑制活性大大提高。通过评估雷帕霉素对从循环CD4 + T细胞离体纯化的明确分化阶段的非调节和Treg群体生长的影响,我们可以证明这种现象不是由于天然Treg的选择性扩增,而是由于雷帕霉素在TCR介导的刺激下诱导常规CD4 + T细胞中的抑制功能。但是,这种情况是暂时的和可逆的,因为它取决于雷帕霉素的持续存在。

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