在这一流行病的发源地喀麦隆,HIV-1 M 组血清系中由 Nef 介导的 HLA-I 和 CD4 分子下调没有发现差异

IF 2 Q4 VIROLOGY
Nelson Sonela, Jaclyn Mann, Celestin Godwe, Oumarou H. Goni, Mérime Tchakoute, Nathalie Nkoue, Tulio de Oliveira, Mark A. Brockman, Zabrina L. Brumme, Thumbi Ndung’u, Marcel Tongo
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摘要

HIV-1 M 组(HIV-1M)病毒株通过其 Nef 蛋白下调 HLA-I 和 CD4 的表达。我们推测,这些 Nef 功能可能是造成疫情中不同品系病毒共同流行的部分原因。在这里,我们描述了来自喀麦隆的 HIV-1M 分离物中这两种 Nef 活性的特征,喀麦隆自疫情爆发以来一直存在多种变体。我们从血浆 HIV RNA 中分离出了生活在喀麦隆偏远村庄和两个国际大都市的 234 名 HIV-1-ART 天真的个体的单个 HIV-1 Nef 克隆,并分析了它们下调 HLA-I 和 CD4 分子的能力。我们发现,尽管存在很大程度的系内和系间差异,但在这些不同的病毒中,Nef下调HLA-I的能力是相似的。此外,Nef 介导的 CD4 下调活性在喀麦隆发现的不同血统中也是完全一致的。此外,我们还观察到一种趋势,即在国际大都市与偏远乡村流行的病毒具有更高的 HLA-I 下调活性,而这两种环境中的 CD4 下调活性相似。此外,我们还注意到,从 2000 年到 2013 年,HLA-I 下调活性显著下降,这为全球 HIV-1M 群体随时间推移而衰减提供了更多证据。最后,我们在 CRF02_AG 优势品系中发现了 18 个与 HLA-I 下调差异相关的氨基酸和 13 个与 CD4 下调差异相关的氨基酸。在 Nef 介导的 HLA-I 和 CD4 下调功能中,我们没有观察到与 HIV 株系相关的差异,这表明这些活动不会对喀麦隆不同 HIV-1M 株系的流行产生实质性影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
No detectable differences in Nef-mediated downregulation of HLA-I and CD4 molecules among HIV-1 group M lineages circulating in Cameroon, where the pandemic originated
HIV-1 group M (HIV-1M) lineages downregulate HLA-I and CD4 expression via their Nef proteins. We hypothesized that these Nef functions may be partially responsible for the differences in prevalence of viruses from different lineages that co-circulate within an epidemic. Here, we characterized these two Nef activities in HIV-1M isolates from Cameroon, where multiple variants have been circulating since the pandemic’s origin. Single HIV-1 Nef clones from 234 HIV-1-ART naïve individuals living in remote villages and two cosmopolitan cities of Cameroon, sampled between 2000 and 2013, were isolated from plasma HIV RNA and analyzed for their capacity to downregulate HLA-I and CD4 molecules. We found that, despite a large degree of within- and inter- lineage variation, the ability of Nef to downregulate HLA-I was similar across these different viruses. Moreover, Nef-mediated CD4 downregulation activity was also well conserved across the different lineages found in Cameroon. In addition, we observed a trend towards higher HLA-I downregulation activity of viruses circulating in the cosmopolitan cities versus the remote villages, whereas the CD4 downregulation activities were similar across the two settings. Furthermore, we noted a significant decline of HLA-I downregulation activity from 2000 to 2013, providing additional evidence supporting the attenuation of the global HIV-1M population over time. Finally, we identified 18 amino acids associated with differential HLA-I downregulation and 13 amino acids associated with differential CD4 downregulation within the dominant CRF02_AG lineage. Our lack of observation of HIV lineage-related differences in Nef-mediated HLA-I and CD4 downregulation function suggests that these activities do not substantively influence the prevalence of different HIV-1M lineages in Cameroon.
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