首页> 美国卫生研究院文献>Journal of Virology >Retroviral Recombination In Vivo: Viral Replication Patterns and Genetic Structure of Simian Immunodeficiency Virus (SIV) Populations in Rhesus Macaques after Simultaneous or Sequential Intravaginal Inoculation with SIVmac239Δvpx/Δvpr and SIVmac239Δnef
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Retroviral Recombination In Vivo: Viral Replication Patterns and Genetic Structure of Simian Immunodeficiency Virus (SIV) Populations in Rhesus Macaques after Simultaneous or Sequential Intravaginal Inoculation with SIVmac239Δvpx/Δvpr and SIVmac239Δnef

机译:体内逆转录病毒重组:在同时或顺序阴道内接种SIVmac239Δvpx/Δvpr和SIVmac239Δnef后恒河猴中的猿猴免疫缺陷病毒(SIV)种群的病毒复制模式和遗传结构

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摘要

To characterize the occurrence, frequency, and kinetics of retroviral recombination in vivo, we intravaginally inoculated rhesus macaques, either simultaneously or sequentially, with attenuated simian immunodeficiency virus (SIV) strains having complementary deletions in their accessory genes and various degrees of replication impairment. In monkeys inoculated simultaneously with SIVmac239Δvpx/Δvpr and SIVmac239Δnef, recombinant wild-type (wt) virus and wild-type levels of plasma viral RNA (vRNA) were detected in blood by 2 weeks postinoculation. In monkeys inoculated first with SIVmac239Δvpx/Δvpr and then with SIVmac239Δnef, recombination occurred but was associated with lower plasma vRNA levels than plasma vRNA levels seen for monkeys inoculated intravaginally with wt SIVmac239. In one monkey, recombination occurred 6 weeks after the challenge with SIVmac239Δnef when plasma SIVmac239Δvpx/Δvpr RNA levels were undetectable. In monkeys inoculated first with the more highly replicating strain, SIVmac239Δnef, and then with SIVmac239Δvpx/Δvpr, wild-type recombinant virus was not detected in blood or tissues. Instead, a virus that had repaired the deletion in the nef gene by a compensatory mutation was found in one animal. Overall, recombinant SIV was eventually found in four of six animals intravaginally inoculated with the two SIVmac239 deletion mutants. These findings show that recombination can occur readily in vivo after mucosal SIV exposure and thus contributes to the generation of viral genetic diversity and enhancement of viral fitness.
机译:为了表征体内逆转录病毒重组的发生,频率和动力学,我们在阴道内恒河猴猕猴同时或依次接种了减毒的猿猴免疫缺陷病毒(SIV)菌株,这些菌株在其辅助基因中具有互补性缺失,并具有不同程度的复制障碍。在同时接种SIVmac239Δvpx/Δvpr和SIVmac239Δnef的猴子中,接种后2周在血液中检测到重组野生型(wt)病毒和血浆病毒RNA(vRNA)的野生型水平。在先接种SIVmac239Δvpx/Δvpr然后再接种SIVmac239Δnef的猴子中,发生了重组,但与血浆vRNA水平较低相关,而血浆vRNA水平低于经阴道内用wt SIVmac239接种的猴子。在一只猴子中,当无法检测到血浆SIVmac239Δvpx/ΔvprRNA水平时,用SIVmac239Δnef攻击后6周发生重组。首先接种高复制株SIVmac239Δnef,然后再接种SIVmac239Δvpx/Δvpr的猴子,在血液或组织中未检测到野生型重组病毒。相反,在一只动物中发现了一种通过补偿性突变修复了nef基因缺失的病毒。总体而言,最终在用两个SIVmac239缺失突变体阴道接种的六只动物中的四只中发现了重组SIV。这些发现表明,在粘膜SIV暴露后,体内重组很容易发生,因此有助于病毒遗传多样性的产生和病毒适应性的增强。

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