HIV Gag 和 Pol 特异性 HLA-B*2705 限制性 CD8+ T 细胞的早期有效抗病毒活性。
Efficacious early antiviral activity of HIV Gag- and Pol-specific HLA-B 2705-restricted CD8+ T cells.
机构信息
Department of Paediatrics, University of Oxford, Peter Medawar Building for Pathogen Research, Oxford OX1 3SY, United Kingdom.
出版信息
J Virol. 2010 Oct;84(20):10543-57. doi: 10.1128/JVI.00793-10. Epub 2010 Aug 4.
The association between HLA-B 2705 and the immune control of human immunodeficiency virus type 1 (HIV-1) has previously been linked to the targeting of the HLA-B 2705-restricted Gag epitope KRWIILGLNK (KK10) by CD8(+) T cells. In order to better define the mechanisms of the HLA-B 2705 immune control of HIV, we first characterized the CD8(+) T-cell responses of nine highly active antiretroviral therapy (HAART)-naïve B 2705-positive subjects. Unexpectedly, we observed a strong response to an HLA-B 2705-restricted Pol epitope, KRKGGIGGY (KY9), in 8/9 subjects. The magnitude of the KY9 response was only marginally lower than that of the KK10-specific response (median, 695 versus 867 spot-forming cells [SFC]/million peripheral blood mononuclear cells [PBMCs]; not significant [NS]), and viral escape mutants were observed in both KY9 and KK10, resulting from selection pressure driven by the respective CD8(+) T-cell response. By comparing inhibitions of viral replication by CD8(+) T cells specific for the Gag KK10, Pol KY9, and Vpr VL9 HLA-B 2705-restricted epitopes, we observed a consistent hierarchy of antiviral efficacy (Gag KK10 > Pol KY9 > Vpr VL9). This hierarchy was associated with early recognition of HIV-1-infected cells, within 6 h of infection, by KK10- and KY9-specific CD8(+) T cells but not until 18 h postinfection by VL9-specific CD8(+) T cells. There was no association between antiviral efficacy and proliferative capacity, cytotoxicity, polyfunctionality, or T-cell receptor (TCR) avidity. These data are consistent with previous studies indicating an important role for the B 2705-Gag KK10 response in the control of HIV but also suggest a previously unrecognized role played by the subdominant Pol-specific KY9 response in HLA-B 2705-mediated control of HIV and that the recognition of HIV-infected cells by CD8(+) T cells early in the viral life cycle may be important for viral containment in HIV-infected individuals.
先前的研究表明,HLA-B2705 与人类免疫缺陷病毒 1(HIV-1)的免疫控制有关,这与 CD8+T 细胞靶向 HLA-B2705 限制性 Gag 表位 KRWIILGLNK(KK10)有关。为了更好地定义 HLA-B2705 对 HIV 的免疫控制机制,我们首先对 9 名未经高效抗逆转录病毒治疗(HAART)的 B2705 阳性受试者的 CD8+T 细胞反应进行了特征描述。出乎意料的是,我们在 8/9 名受试者中观察到了对 HLA-B2705 限制性 Pol 表位 KRKGGIGGY(KY9)的强烈反应。KY9 反应的强度仅略低于 KK10 特异性反应(中位数,695 与 867 个斑点形成细胞[SFC]/百万外周血单核细胞[PBMC];无显著性[NS]),并且在 KY9 和 KK10 中都观察到了病毒逃逸突变体,这是由各自的 CD8+T 细胞反应驱动的选择压力导致的。通过比较针对 Gag KK10、Pol KY9 和 Vpr VL9 HLA-B2705 限制性表位的 CD8+T 细胞对病毒复制的抑制作用,我们观察到抗病毒功效的一致等级(Gag KK10 > Pol KY9 > Vpr VL9)。这种等级与 KK10 和 KY9 特异性 CD8+T 细胞在感染后 6 小时内对 HIV-1 感染细胞的早期识别有关,但 VL9 特异性 CD8+T 细胞直到感染后 18 小时才出现。抗病毒功效与增殖能力、细胞毒性、多功能性或 T 细胞受体(TCR)亲和力之间没有关联。这些数据与先前的研究一致,表明 B2705-Gag KK10 反应在控制 HIV 中起着重要作用,但也表明以前未被认识到的亚优势 Pol 特异性 KY9 反应在 HLA-B2705 介导的 HIV 控制中发挥作用,并且 CD8+T 细胞在病毒生命周期早期对 HIV 感染细胞的识别可能对 HIV 感染者的病毒控制很重要。
Zotero 插件