首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Neutralizing antibody responses drive the evolution of human immunodeficiency virus type 1 envelope during recent HIV infection.
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Neutralizing antibody responses drive the evolution of human immunodeficiency virus type 1 envelope during recent HIV infection.

机译:在最近的HIV感染过程中,中和性抗体反应可驱动1型人类免疫缺陷病毒包膜的进化。

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HIV type 1 (HIV-1) can rapidly escape from neutralizing antibody responses. The genetic basis of this escape in vivo is poorly understood. We compared the pattern of evolution of the HIV-1 env gene between individuals with recent HIV infection whose virus exhibited either a low or a high rate of escape from neutralizing antibody responses. We demonstrate that the rate of viral escape at a phenotypic level is highly variable among individuals, and is strongly correlated with the rate of amino acid substitutions. We show that dramatic escape from neutralizing antibodies can occur in the relative absence of changes in glycosylation or insertions and deletions ("indels") in the envelope; conversely, changes in glycosylation and indels occur even in the absence of neutralizing antibody responses. Comparison of our data with the predictions of a mathematical model support a mechanism in which escape from neutralizing antibodies occurs via many amino acid substitutions, with low cross-neutralization between closely related viral strains. Our results suggest that autologous neutralizing antibody responses may play a pivotal role in the diversification of HIV-1 envelope during the early stages of infection.
机译:1型HIV(HIV-1)可以迅速中和抗体反应。体内逃逸的遗传基础了解甚少。我们比较了HIV-1 env基因在最近感染HIV的个体之间的进化模式,该个体的病毒表现出中和抗体应答的逃逸率低或高。我们证明,在表型水平上病毒逃逸的速率在个体之间是高度可变的,并且与氨基酸取代的速率密切相关。我们表明,在相对不存在糖基化变化或包膜中插入和缺失(“ indels”)的情况下,可以发生中和抗体的戏剧性逃逸。相反,即使没有中和抗体反应,糖基化和插入缺失的变化也会发生。我们的数据与数学模型的预测结果的比较支持了一种机制,其中中和抗体的逃逸是通过许多氨基酸取代发生的,而密切相关的病毒株之间的交叉中和性较低。我们的结果表明自体中和抗体反应可能在感染的早期阶段在HIV-1包膜的多样化中起关键作用。

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