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Lack of CD28 expression on HIV-specific cytotoxic T lymphocytes is associated with disease progression.

机译:HIV特异性细胞毒性T淋巴细胞缺乏CD28表达与疾病进展有关。

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摘要

During HIV infection, CD8+ T cells lacking the costimulatory molecule CD28 increase in number and proportion. This accumulation is associated with disease activity and possibly with CD8+ T-cell dysfunction. In this study, CD8+CD28+ and CD8+CD28- T cells from 41 HIV-infected individuals at various stages of disease were compared in terms of HIV-specific cytotoxicity, TCRbetaV repertoire diversity, and cytokine production. We found that the CD28 phenotype of anti-HIV CTL evolves in parallel with disease progression and disease activity. Absolute numbers of CD4+ T cells and CD4+/CD8+ T-cell ratios progressively decreased in 3 groups with an increasing prevalence of CD28- HIV-specific CTL. Conversely, HIV replication levels progressively increased in parallel with the prevalence of CD28- HIV-specific CTL. Repertoire diversity at the level of TCRbetaV gene family expression was maintained at normal levels for both CD28+ and CD28- T cells at all stages of infection. Diversity at the level of junctional length polymorphism was more restricted in the CD8+CD28- T-cell population, but this difference remained relatively constant through different stages of infection. Both CD28+ and CD28- T cells produced IL-2 and IFN-gamma, regardless of disease stage and/or the predominant CD28 phenotype of anti-HIV CTL.
机译:在HIV感染期间,缺少共刺激分子CD28的CD8 + T细胞的数量和比例增加。这种积累与疾病活动以及可能与CD8 + T细胞功能障碍有关。在这项研究中,比较了41个处于不同疾病阶段的HIV感染者的CD8 + CD28 +和CD8 + CD28-T细胞的HIV特异性细胞毒性,TCRbetaV谱系多样性和细胞因子产生。我们发现抗HIV CTL的CD28表型与疾病进展和疾病活动同时发生。随着CD28-HIV特异性CTL的患病率增加,3组中CD4 + T细胞的绝对数量和CD4 + / CD8 + T细胞比率逐渐降低。相反,HIV复制水平与CD28-HIV特异性CTL的流行同时增加。在感染的所有阶段,CD28 +和CD28-T细胞的TCRbetaV基因家族表达水平的库多样性均保持在正常水平。在连接长度多态性水平上的多样性在CD8 + CD28-T细胞群体中受到更多限制,但是这种差异在感染的不同阶段保持相对恒定。不论疾病阶段和/或抗HIV CTL的主要CD28表型如何,CD28 +和CD28- T细胞均产生IL-2和IFN-γ。

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