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Loss of HIV-1–specific CD8+ T Cell Proliferation after Acute HIV-1 Infection and Restoration by Vaccine-induced HIV-1–specific CD4+ T Cells

机译:急性HIV-1感染和疫苗诱导的HIV-1特异性CD4 + T细胞恢复后,HIV-1特异性CD8 + T细胞增殖的丧失

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摘要

Virus-specific CD8+ T cells are associated with declining viremia in acute human immunodeficiency virus (HIV)1 infection, but do not correlate with control of viremia in chronic infection, suggesting a progressive functional defect not measured by interferon γ assays presently used. Here, we demonstrate that HIV-1–specific CD8+ T cells proliferate rapidly upon encounter with cognate antigen in acute infection, but lose this capacity with ongoing viral replication. This functional defect can be induced in vitro by depletion of CD4+ T cells or addition of interleukin 2–neutralizing antibodies, and can be corrected in chronic infection in vitro by addition of autologous CD4+ T cells isolated during acute infection and in vivo by vaccine-mediated induction of HIV-1–specific CD4+ T helper cell responses. These data demonstrate a loss of HIV-1–specific CD8+ T cell function that not only correlates with progressive infection, but also can be restored in chronic infection by augmentation of HIV-1–specific T helper cell function. This identification of a reversible defect in cell-mediated immunity in chronic HIV-1 infection has important implications for immunotherapeutic interventions.
机译:病毒特异性CD8 + T细胞与急性人类免疫缺陷病毒(HIV)1感染中病毒血症的下降有关,但与慢性感染中病毒血症的控制无关,表明目前尚无法通过干扰素γ测定法检测到的进行性功能缺陷。在这里,我们证明了在急性感染中遇到同源抗原后,HIV-1特异性CD8 + T细胞迅速增殖,但随着病毒的复制而失去这种能力。这种功能性缺陷可以在体外通过耗尽CD4 + T细胞或添加白介素2中和抗体来诱导,并且可以在慢性感染中通过添加急性感染过程中分离的自体CD4 + T细胞以及在体内通过疫苗介导的方法加以纠正。诱导HIV-1特异性CD4 + T辅助细胞应答。这些数据表明,HIV-1特异性CD8 + T细胞功能的丧失不仅与进行性感染有关,而且在慢性感染中可以通过增强HIV-1特异性T辅助细胞功能来恢复。慢性HIV-1感染中细胞介导的免疫可逆缺陷的这种鉴定对免疫治疗干预具有重要意义。

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