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Perturbation of CD4+ and CD8+ T-cell repertoires during progression to AIDS and regulation of the CD4+ repertoire during antiviral therapy (see comments)

机译:在发展为艾滋病期间,CD4 +和CD8 + T细胞库的摄动,以及在抗病毒治疗期间对CD4 + T细胞库的调节(见评论)

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摘要

The T-cell antigen receptor (TCR) repertoire was studied longitudinally by analyzing the varying lengths of the beta chain CDR3 hypervariable region during the course of HIV-1 infection and following combination antiretroviral therapy. Drastic restrictions in CD8+ T-cell repertoire usage were found at all stages of natural progression and persisted during the first six months of treatment. In contrast, significant CD4+ T-cell repertoire perturbations were not found in early stages of infection but correlated with progression to AIDS. Out of ten patients presenting with pretreatment perturbations, normalization of the CD4+ repertoire was observed in eight good responders, but not in two cases of unsuccessful therapy. These results indicate that, besides CD4+ cell count rise, an efficient control of HIV replication may allow qualitative modifications of the CD4+ repertoire balance.
机译:通过分析HIV-1感染过程中以及联合抗逆转录病毒疗法后β链CDR3高变区的不同长度,纵向研究了T细胞抗原受体(TCR)库。在自然发展的所有阶段都发现CD8 + T细胞库使用受到严重限制,并在治疗的前六个月持续存在。相比之下,在感染的早期阶段未发现明显的CD4 + T细胞库扰动,但与艾滋病进展相关。在十名表现出治疗前摄动的患者中,在八名良好反应者中观察到CD4 +谱库正常,但在两例治疗失败的病例中未观察到。这些结果表明,除了CD4 +细胞数量增加之外,对HIV复制的有效控制还可能使CD4 +曲目库平衡发生质的改变。

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