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具有保护性干扰素调节因子-1基因型的受试者中HIV-1长末端重复序列转录减少:一种介导对HIV-1感染抗性的潜在机制。

Reduced HIV-1 long terminal repeat transcription in subjects with protective interferon regulatory factor-1 genotype: a potential mechanism mediating resistance to infection by HIV-1.

作者信息

Ji Hezhao, Ball Terry Blake, Ao Zhujun, Kimani Joshua, Yao Xiaojian, Plummer Francis Allan

机构信息

Department of Medical Microbiology and Infectious Diseases, University of Manitoba, Winnipeg, Manitoba, Canada.

出版信息

Scand J Infect Dis. 2010 May;42(5):389-94. doi: 10.3109/00365540903496536.

DOI:10.3109/00365540903496536
PMID:20100115
Abstract

We previously described the polymorphism in the interferon regulatory factor-1 (IRF-1) gene as a novel correlate of resistance to HIV-1 infection in a Kenyan female sex worker cohort. However, the underlying mechanisms likely mediating this association remained to be elucidated. The initiation of HIV-1 long terminal repeat (LTR) transcription in peripheral blood mononuclear cells (PBMCs) from subjects with different IRF-1 haplotypes, representing protective, intermediate and the least protective IRF-1 allele combinations, were investigated here. A single-cycle pseudovirus construct expressing vesicular stomatitis virus envelop G-protein (VSV-G) and having an HIV-1 pNL4.3 backbone with luciferase insert was used to infect PBMCs with different IRF-1 haplotypes. The efficiency of early HIV-1 LTR transcription was monitored using a luciferase assay. IRF-1 protein levels induced by the infection were measured by quantitative Western blot. Our results showed that PBMCs with the protective IRF-1 genotype demonstrated significantly lower HIV-1 LTR transcription during the initial stages of infection compared to PBMCs with other haplotypes, which correlated with the kinetics of IRF-1 responsiveness to HIV-1 infection in the cells. It suggests that IRF-1 genotypes alter the efficiency of early HIV-1 LTR transcription, likely via modulating expression of IRF-1. This may represent one mechanism mediating the association between IRF-1 polymorphisms and resistance to HIV-1 infection.

摘要

我们之前曾描述过,在肯尼亚女性性工作者队列中,干扰素调节因子-1(IRF-1)基因的多态性是对HIV-1感染产生抗性的一种新关联。然而,可能介导这种关联的潜在机制仍有待阐明。在此,我们研究了来自具有不同IRF-1单倍型(代表保护性、中间性和最低保护性IRF-1等位基因组合)的受试者外周血单核细胞(PBMC)中HIV-1长末端重复序列(LTR)转录的起始情况。使用一种表达水疱性口炎病毒包膜糖蛋白(VSV-G)且具有带有荧光素酶插入片段的HIV-1 pNL4.3骨架的单周期假病毒构建体来感染具有不同IRF-1单倍型的PBMC。使用荧光素酶测定法监测早期HIV-1 LTR转录的效率。通过定量蛋白质免疫印迹法测量感染诱导的IRF-1蛋白水平。我们的结果表明,与具有其他单倍型的PBMC相比,具有保护性IRF-1基因型的PBMC在感染初始阶段显示出显著更低的HIV-1 LTR转录,这与细胞中IRF-1对HIV-1感染的反应动力学相关。这表明IRF-1基因型可能通过调节IRF-1的表达来改变早期HIV-1 LTR转录的效率。这可能代表了一种介导IRF-1多态性与对HIV-1感染抗性之间关联的机制。

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