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首页> 外文期刊>Antiviral therapy >IL-7/IL-7 receptor system regulation following IL-2 immunotherapy in HIV-infected patients.
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IL-7/IL-7 receptor system regulation following IL-2 immunotherapy in HIV-infected patients.

机译:在HIV感染的患者中进行IL-2免疫治疗后,IL-7 / IL-7受体系统的调节。

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摘要

Interleukin-2 (IL-2) and IL-7 are the most intriguing molecules in immune-based HIV infection treatment. An in vitro IL-2/IL-7 cross-talk due to IL-2-driven IL-7 receptor-alpha-chain (IL-7R alpha) down-modulation, potentially blocking IL-7 signalling has been described. We investigated the in vivo IL-2 effect on IL-7/IL-7R system, measuring free IL-7, and IL-7R alpha CD4 and CD8 in 12 HIV-positive patients enrolled in a randomized IL-2 trial. Compared to HAART alone, IL-2 induced a parallel expansion in total and naive CD4, TRECs and IL-7 plasma levels, with no IL-7R alpha CD4 and IL-7R alpha CD8 changes (P>0.05), suggesting that in vivo IL-2 boosts IL-7 production without down-modulating IL-7R alpha, preserving IL-7-mediated T-lymphocyte homeostatic regulation. Our data confirm the pivotal role of IL-2 and IL-7 in the regulation of T-lymphocyte homeostasis in HIV infection.
机译:在基于免疫的HIV感染治疗中,白介素2(IL-2)和IL-7是最吸引人的分子。已经描述了由于IL-2驱动的IL-7受体-α链(IL-7R alpha)下调导致的体外IL-2 / IL-7串扰,可能会阻断IL-7信号传导。我们调查了参加随机IL-2试验的12名HIV阳性患者的体内IL-2对IL-7 / IL-7R系统的影响,测量了游离IL-7和IL-7R alpha CD4和CD8。与单独的HAART相比,IL-2诱导了总和天然CD4,TRECs和IL-7血浆水平的平行扩展,而IL-7R alpha CD4和IL-7R alpha CD8没有变化(P> 0.05),这表明体内IL-2在不下调IL-7Rα的情况下提高IL-7的产生,从而保持IL-7介导的T淋巴细胞稳态调节。我们的数据证实了IL-2和IL-7在调节HIV感染T淋巴细胞稳态中的关键作用。

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