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Infection of CD8+CD45RO+ Memory T-Cells by HIV-1 and Their Proliferative Response

机译:HIV-1对CD8 + CD45RO +记忆T细胞的感染及其增殖反应

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摘要

CD8+ T-cells are involved in controlling HIV-1 infection by eliminating infected cells and secreting soluble factors that inhibit viral replication. To investigate the mechanism and significance of infection of CD8+ T-cells by HIV-1 in vitro, we examined the susceptibility of these cells and their subsets to infection. CD8+ T-cells supported greater levels of replication with T-cell tropic strains of HIV-1, though viral production was lower than that observed in CD4+ T-cells. CD8+ T-cell infection was found to be productive through ELISA, RT-PCR and flow cytometric analyses. In addition, the CD8+CD45RO+ memory T-cell population supported higher levels of HIV-1 replication than CD8+CD45RA+ naïve T-cells. However, infection of CD8+CD45RO+ T-cells did not affect their proliferative response to the majority of mitogens tested. We conclude, with numerous lines of evidence detecting and measuring infection of CD8+ T-cells and their subsets, that this cellular target and potential reservoir may be central to HIV-1 pathogenesis.
机译:CD8 + T细胞通过消除受感染的细胞并分泌抑制病毒复制的可溶性因子参与控制HIV-1感染。为了研究HIV-1在体外感染CD8 + T细胞的机制和意义,我们检查了这些细胞及其亚群对感染的敏感性。 CD8 + T细胞支持HIV-1的T细胞嗜性株复制的水平更高,尽管病毒产量低于CD4 + T细胞中观察到的。通过ELISA,RT-PCR和流式细胞仪分析发现CD8 + T细胞感染具有生产力。另外,CD8 + CD45RO +记忆性T细胞群体比CD8 + CD45RA +幼稚T细胞支持更高水平的HIV-1复制。但是,CD8 + CD45RO + T细胞的感染不会影响它们对大多数测试的有丝分裂原的增殖反应。我们得出的结论是,根据众多检测和测量CD8 + T细胞及其亚群感染的证据,该细胞靶标和潜在储库可能是HIV-1发病机制的核心。

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