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与 HIV-1/M 和 HIV-1/O 亲本病毒相比,HIV-1/MO 重组病毒在体外的复制潜力。

In vitro replicative potential of an HIV-1/MO intergroup recombinant virus compared to HIV-1/M and HIV-1/O parental viruses.

机构信息

Univ Rouen Normandie, Université de Caen Normandie, INSERM, Normandie Univ, DYNAMICURE UMR 1311, CHU Rouen, Department of Virology, National Reference Center of HIV, 76000, Rouen, France.

Univ Rouen Normandie, Université de Caen Normandie, INSERM, Normandie Univ, DYNAMICURE UMR 1311, 76000, Rouen, France.

出版信息

Sci Rep. 2024 Jan 19;14(1):1730. doi: 10.1038/s41598-024-51873-3.

Abstract

Genetic recombination is one of the major evolution processes of HIV-1. Despite their great genetic divergence, HIV-1 groups M and O can generate HIV-1/MO intergroup recombinants. The current description of 20 HIV-1/MO unique recombinant forms suggests a possible benefit of the recombination. The aim of this work was to study in vitro the replicative potential of HIV-1/MO recombinant forms. This analysis was based on a simple recombination pattern, [O-M], harboring a breakpoint in Vpr. A chimeric infectious molecular clone, pOM-TB-2016 was synthesized from HIV-1/M subtype B and HIV-1/O subgroup T and recombinant viruses were obtained by transfection/co-culture. To compare the replicative potential of these viruses, two markers were monitored in culture supernatants: Reverse Transcriptase (RT) activity and P24 antigen concentration. The results showed a superiority of the group M parental virus compared to group O for both markers. In contrast, for the recombinant virus, RT activity data did not overlap with the concentration of P24 antigen, suggesting a hybrid behavior of the recombinant, in terms of enzyme activity and P24 production. These results highlighted many hypotheses about the impact of recombination on replicative potential and demonstrated again the significant plasticity of HIV genomes and their infinite possibility of evolution.

摘要

遗传重组是 HIV-1 的主要进化过程之一。尽管 HIV-1 组 M 和 O 具有很大的遗传差异,但它们可以产生 HIV-1/MO 重组体。目前对 20 种 HIV-1/MO 独特重组形式的描述表明重组可能具有益处。本研究旨在体外研究 HIV-1/MO 重组形式的复制潜力。该分析基于一种简单的重组模式 [O-M],其中包含 Vpr 中的断点。从 HIV-1/M 亚型 B 和 HIV-1/O 亚组 T 合成嵌合感染性分子克隆 pOM-TB-2016,并通过转染/共培养获得重组病毒。为了比较这些病毒的复制潜力,在培养上清液中监测了两个标记物:逆转录酶(RT)活性和 P24 抗原浓度。结果表明,与 HIV-1/O 组相比,两种标记物均显示组 M 亲本病毒具有优势。相比之下,对于重组病毒,RT 活性数据与 P24 抗原浓度不重叠,这表明重组病毒在酶活性和 P24 产生方面具有混合行为。这些结果提出了许多关于重组对复制潜力的影响的假设,并再次证明了 HIV 基因组的显著可塑性及其无限的进化可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a33/10799055/89683ffbed58/41598_2024_51873_Fig1_HTML.jpg

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