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包膜疫苗接种塑造恒河猴感染猴免疫缺陷病毒后的病毒包膜进化。

Envelope vaccination shapes viral envelope evolution following simian immunodeficiency virus infection in rhesus monkeys.

机构信息

Division of Viral Pathogenesis, Department of Medicine, Beth Israel Deaconess Medical Center, Harvard Medical School, 330 Brookline Avenue, Boston, MA 02215, USA.

出版信息

J Virol. 2010 Jan;84(2):953-63. doi: 10.1128/JVI.01679-09. Epub 2009 Nov 11.

Abstract

The evolution of envelope mutations by replicating primate immunodeficiency viruses allows these viruses to escape from the immune pressure mediated by neutralizing antibodies. Vaccine-induced anti-envelope antibody responses may accelerate and/or alter the specificity of the antibodies, thus shaping the evolution of envelope mutations in the replicating virus. To explore this possibility, we studied the neutralizing antibody response and the envelope sequences in rhesus monkeys vaccinated with either gag-pol-nef immunogens or gag-pol-nef immunogens in combination with env and then infected with simian immunodeficiency virus (SIV). Using a pseudovirion neutralization assay, we demonstrate that envelope vaccination primed for an accelerated neutralizing antibody response following virus challenge. To monitor viral envelope evolution in these two cohorts of monkeys, full-length envelopes from plasma virus isolated at weeks 37 and 62 postchallenge were sequenced by single genome amplification to identify sites of envelope mutations. We show that env vaccination was associated with a change in the pattern of envelope mutations. Prevalent mutations in sequences from gag-pol-nef vaccinees included deletions in both variable regions 1 and 4 (V1 and V4), whereas deletions in the env vaccinees occurred only in V1. These data show that env vaccination altered the focus of the antibody-mediated selection pressure on the evolution of envelope following SIV challenge.

摘要

复制灵长类免疫缺陷病毒的包膜突变的进化使这些病毒能够逃避中和抗体介导的免疫压力。疫苗诱导的抗包膜抗体反应可能会加速和/或改变抗体的特异性,从而塑造复制病毒中包膜突变的进化。为了探索这种可能性,我们研究了恒河猴接种 gag-pol-nef 免疫原或 gag-pol-nef 免疫原与 env 联合免疫后感染猿猴免疫缺陷病毒(SIV)的中和抗体反应和包膜序列。我们使用假病毒中和测定法证明,包膜疫苗接种可在病毒攻击后加速产生中和抗体反应。为了监测这两组猴子中病毒包膜的进化,我们通过单基因组扩增对血浆病毒中分离的第 37 周和第 62 周的全长包膜进行了测序,以鉴定包膜突变的部位。我们发现,env 疫苗接种与包膜突变模式的变化有关。在 gag-pol-nef 疫苗接种者的序列中,常见的突变包括 V1 和 V4 两个可变区的缺失,而在 env 疫苗接种者中,缺失仅发生在 V1 中。这些数据表明,env 疫苗接种改变了 SIV 攻击后抗体介导的选择压力对包膜进化的重点。

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