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在中国的长期存活的 HIV-1 感染前血浆供者中,Gag 的 CTL 靶向优先与相对病毒控制相关。

Preferential CTL targeting of Gag is associated with relative viral control in long-term surviving HIV-1 infected former plasma donors from China.

机构信息

State Key Laboratory for Infectious Disease Prevention and Control, National Center for AIDS/STD Control and Prevention, Chinese Center for Disease Control and Prevention, Beijing 102206, China.

出版信息

Cell Res. 2012 May;22(5):903-14. doi: 10.1038/cr.2012.19. Epub 2012 Jan 31.

Abstract

It is generally believed that CD8(+) cytotoxic T lymphocytes (CTLs) play a critical role in limiting the replication of human immunodeficiency virus type 1 (HIV-1) and in determining the outcome of the infection, and this effect may partly depend on which HIV product is preferentially targeted. To address the correlation between HIV-1-specific CTL responses and virus replication in a cohort of former plasma donors (FPDs), 143 antiretroviral therapy naive FPDs infected with HIV-1 clade B' strains were assessed for HIV-1-specific CTL responses with an IFN-γ Elispot assay at single peptide level by using overlapping peptides (OLPs) covering the whole consensus clade B proteome. By using a Spearman's rank correlation analysis, we found that the proportion of Gag-specific CTL responses among the total virus-specific CTL activity was inversely correlated with viral loads while being positively correlated to CD4 counts, as opposed to Pol- and Env-specific responses that were associated with increased viral loads and decreased CD4 counts. In addition, Vpr-specifc CTL responses showed a similar protective effect with Gag responses, but with a much lower frequency of recognition. Significantly, we also observed an association between HLA-A30/B13/Cw06 haplotype and lower viral loads that was probably due to restricted Gag-specific CTL responses. Thus, our data demonstrate the prominent role of Gag-specific CTL responses in disease control. The advantage of HLA-A30/B13/Cw06 haplotype in viral control may be associated with the contribution of Gag-specific CTL responses in the studied individuals.

摘要

普遍认为,CD8(+)细胞毒性 T 淋巴细胞(CTL)在限制人类免疫缺陷病毒 1(HIV-1)的复制和决定感染结果方面起着关键作用,这种作用可能部分取决于 HIV 产物的优先靶向。为了在以前的血浆供体(FPD)队列中研究 HIV-1 特异性 CTL 反应与病毒复制之间的相关性,对 143 名未经抗逆转录病毒治疗的 HIV-1 分 B' 株感染的 FPD 进行了 HIV-1 特异性 CTL 反应评估,采用 IFN-γ Elispot 测定法,在单个肽水平上,使用覆盖整个共识 B 族蛋白组的重叠肽(OLP)进行。通过 Spearman 秩相关分析,我们发现,Gag 特异性 CTL 反应在总病毒特异性 CTL 活性中的比例与病毒载量呈负相关,而与 CD4 计数呈正相关,而 Pol 和 Env 特异性反应则与病毒载量增加和 CD4 计数降低相关。此外,Vpr 特异性 CTL 反应表现出与 Gag 反应相似的保护作用,但识别频率要低得多。值得注意的是,我们还观察到 HLA-A30/B13/Cw06 单倍型与较低病毒载量之间存在关联,这可能是由于受限制的 Gag 特异性 CTL 反应所致。因此,我们的数据表明 Gag 特异性 CTL 反应在疾病控制中的突出作用。HLA-A30/B13/Cw06 单倍型在病毒控制方面的优势可能与研究个体中 Gag 特异性 CTL 反应的贡献有关。

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