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A strongly selected mutation in the HIV-1 genome is independent of T cell responses and neutralizing antibodies

机译:HIV-1基因组中的强烈选择的突变独立于T细胞应答和中和抗体

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摘要

Background: Mutations rapidly accumulate in the HIV-1 genome after infection. Some of those mutations are selected by host immune responses and often cause viral ftness losses. This study is to investigate whether strongly selected mutations that are not associated with immune responses result in ftness losses. Results: Strongly selected mutations were identifed by analyzing 5′-half HIV-1 genome (gag/pol) sequences from longitudinal samples of subject CH0131. The K43R mutation in the gag gene was frst detected at day 91 post screening and was fxed in the viral population at day 273 while the synonymous N323tc mutation was frst detected at day 177 and fxed at day 670. No conventional or cryptic T cell responses were detected against either mutation sites by ELISpot analysis. However, when ftness costs of both mutations were measured by introducing each mutation into their cognate transmitted/founder (T/F) viral genome, the K43R mutation caused a signifcant ftness loss while the N323tc mutation had little impact on viral ftness. Conclusions: The rapid fxation, the lack of detectable immune responses and the signifcant ftness cost of the K43R mutation suggests that it was strongly selected by host factors other than T cell responses and neutralizing antibodies
机译:背景:感染后,突变在HIV-1基因组中迅速积累。这些突变中的一些是通过宿主免疫反应选择的,通常会导致病毒感染。这项研究旨在调查与免疫反应不相关的强烈选择的突变是否会导致虚弱。结果:通过分析对象CH0131的纵向样本中的5'-一半HIV-1基因组(gag / pol)序列,可以确定强烈选择的突变。在筛选后的第91天首先检测到gag基因中的K43R突变,并在第273天在病毒种群中修复,而同义N323tc突变在177天时发现并在670天时修复。没有传统或隐秘的T细胞反应通过ELISpot分析针对任一突变位点检测到。但是,当通过将每个突变引入其同源的传播/建立者(T / F)病毒基因组来测量两个突变的实足性成本时,K43R突变导致明显的实足性丧失,而N323tc突变对病毒实足性的影响很小。结论:快速固定,缺乏可检测的免疫反应以及K43R突变的明显成本,表明它是受T细胞反应和中和抗体以外的宿主因素强烈选择的

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