HLA-B*81 相关突变对 HIV-1 Gag 复制能力的影响。

Impact of HLA-B*81-associated mutations in HIV-1 Gag on viral replication capacity.

机构信息

HIV Pathogenesis Programme, Doris Duke Medical Research Institute, Nelson R. Mandela School of Medicine, University of KwaZulu-Natal, Durban, South Africa.

出版信息

J Virol. 2012 Mar;86(6):3193-9. doi: 10.1128/JVI.06682-11. Epub 2012 Jan 11.

DOI:10.1128/JVI.06682-11

PMID:22238317

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3302318/

Abstract

HIV-1 attenuation resulting from immune escape mutations selected in Gag may contribute to slower disease progression in HIV-1-infected individuals expressing certain HLA class I alleles. We previously showed that the protective allele HLA-B81 and the HLA-B81-selected Gag T186S mutation are strongly associated with a lower viral replication capacity of recombinant viruses encoding Gag-protease derived from individuals chronically infected with HIV-1 subtype C. In the present study, we directly tested the effect of this mutation on viral replication capacity. In addition, we investigated potential compensatory effects of various polymorphisms, including other HLA-B81-associated mutations that significantly covary with the T186S mutation. Mutations were introduced into a reference subtype B backbone and into patient-derived subtype C sequences in subtype B and C backbones by site-directed mutagenesis. The exponential-phase growth of mutant and wild-type viruses was assayed by flow cytometry of a green fluorescent protein reporter T cell line or by measurement of HIV-1 reverse transcriptase activity in culture supernatants. Engineering of the T186S mutation alone into all patient-derived subtype C sequences failed to yield replication-competent viruses, while in the subtype B sequence, the T186S mutation resulted in impaired replication capacity. Only the T186S mutation in combination with the T190I mutation yielded replication-competent viruses for all virus backbones tested; however, these constructs replicated slower than the wild type, suggesting that only partial compensation is mediated by the T190I mutation. Constructs encoding the T186S mutation in combination with other putative compensatory mutations were attenuated or defective. These results suggest that the T186S mutation is deleterious to HIV-1 subtype C replication and likely requires complex compensatory pathways, which may contribute to the clinical benefit associated with HLA-B81.

摘要

HIV-1 包膜糖蛋白（Gag）中免疫逃逸突变导致的衰减可能有助于表达特定 HLA Ⅰ类等位基因的 HIV-1 感染者疾病进展缓慢。我们先前的研究表明，保护性等位基因 HLA-B81 和 HLA-B81 选择的 Gag T186S 突变与 HIV-1 慢性感染者 Gag-蛋白酶编码重组病毒的复制能力较低强烈相关。在本研究中，我们直接测试了该突变对病毒复制能力的影响。此外，我们研究了各种多态性的潜在补偿效应，包括与 T186S 突变显著相关的其他 HLA-B81 相关突变。通过定点诱变，在参考亚型 B 骨架中以及在亚型 B 和 C 骨架中的患者来源的亚型 C 序列中引入突变。通过绿色荧光蛋白报告 T 细胞系的流式细胞术或通过在培养上清液中测量 HIV-1 逆转录酶活性，检测突变体和野生型病毒的指数期生长。在所有患者来源的亚型 C 序列中单独构建 T186S 突变不能产生复制能力的病毒，而在亚型 B 序列中，T186S 突变导致复制能力受损。仅 T186S 突变与 T190I 突变的组合在所有测试的病毒骨架中产生复制能力的病毒；然而，这些构建体的复制速度比野生型慢，表明仅部分补偿是由 T190I 突变介导的。编码 T186S 突变与其他假定补偿性突变组合的构建体被削弱或缺陷。这些结果表明，T186S 突变对 HIV-1 亚型 C 的复制具有有害影响，可能需要复杂的补偿途径，这可能有助于与 HLA-B81 相关的临床益处。

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