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将 HLA-HIV 关联转移到细胞水平:HIV 适应于扩大针对 Nef 和 HLA 适应变体表位的 CD8 T 细胞反应。

Translation of HLA-HIV associations to the cellular level: HIV adapts to inflate CD8 T cell responses against Nef and HLA-adapted variant epitopes.

机构信息

Centre for Clinical Immunology and Biomedical Statistics, Institute for Immunology and Infectious Diseases, Murdoch University, Murdoch, Western Australia 6150, Australia.

出版信息

J Immunol. 2011 Sep 1;187(5):2502-13. doi: 10.4049/jimmunol.1100691. Epub 2011 Aug 5.

Abstract

Strong statistical associations between polymorphisms in HIV-1 population sequences and carriage of HLA class I alleles have been widely used to identify possible sites of CD8 T cell immune selection in vivo. However, there have been few attempts to prospectively and systematically test these genetic hypotheses arising from population-based studies at a cellular, functional level. We assayed CD8 T cell epitope-specific IFN-γ responses in 290 individuals from the same cohort, which gave rise to 874 HLA-HIV associations in genetic analyses, taking into account autologous viral sequences and individual HLA genotypes. We found immunological evidence for 58% of 374 associations tested as sites of primary immune selection and identified up to 50 novel HIV-1 epitopes using this reverse-genomics approach. Many HLA-adapted epitopes elicited equivalent or higher-magnitude IFN-γ responses than did the nonadapted epitopes, particularly in Nef. At a population level, inclusion of all of the immunoreactive variant CD8 T cell epitopes in Gag, Pol, Nef, and Env suggested that HIV adaptation leads to an inflation of Nef-directed immune responses relative to other proteins. We concluded that HLA-HIV associations mark viral epitopes subject to CD8 T cell selection. These results can be used to guide functional studies of specific epitopes and escape mutations, as well as to test, train, and evaluate analytical models of viral escape and fitness. The inflation of Nef and HLA-adapted variant responses may have negative effects on natural and vaccine immunity against HIV and, therefore, has implications for diversity coverage approaches in HIV vaccine design.

摘要

HIV-1 群体序列中的多态性与 HLA Ⅰ类等位基因携带之间存在强烈的统计学关联,这已被广泛用于鉴定体内 CD8 T 细胞免疫选择的可能位点。然而,很少有尝试从基于人群的研究中,在细胞和功能水平上前瞻性和系统地检验这些遗传假设。我们在同一队列的 290 名个体中检测了 CD8 T 细胞表位特异性 IFN-γ 反应,这些个体的遗传分析产生了 874 个 HLA-HIV 关联,同时考虑了自体病毒序列和个体 HLA 基因型。我们发现,在 374 个经测试的关联中有 58%是作为原发性免疫选择的位点,并且使用这种反向基因组学方法鉴定了多达 50 个新的 HIV-1 表位。许多 HLA 适应的表位引起的 IFN-γ 反应与非适应的表位相当或更高,特别是在 Nef 中。在群体水平上,将 gag、pol、nef 和 env 中所有有免疫反应的变异 CD8 T 细胞表位都包括在内,表明 HIV 的适应导致相对于其他蛋白,Nef 定向免疫反应的膨胀。我们得出结论,HLA-HIV 关联标记了受 CD8 T 细胞选择的病毒表位。这些结果可用于指导对特定表位和逃逸突变的功能研究,以及检验、训练和评估 HIV 逃逸和适应性的分析模型。Nef 和 HLA 适应的变异体反应的膨胀可能对 HIV 的自然和疫苗免疫产生负面影响,因此对 HIV 疫苗设计中的多样性覆盖方法具有重要意义。

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本文引用的文献

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