在 gp120 的 C4 区的单个氨基酸取代通过调节 CD4 结合位点和 V3 环赋予增强的 HIV-1 中和能力。
A single amino acid substitution in the C4 region in gp120 confers enhanced neutralization of HIV-1 by modulating CD4 binding sites and V3 loop.
机构信息
Department of Molecular Virology, National AIDS Research Institute, Pune, India.
出版信息
Virology. 2011 Sep 30;418(2):123-32. doi: 10.1016/j.virol.2011.07.015. Epub 2011 Aug 17.
Abstract
Identification of vulnerability in the HIV-1 envelope (Env) will aid in Env-based vaccine design. We recently found an HIV-1 clade C Env clone (4-2.J45) amplified from a recently infected Indian patient showing exceptional neutralization sensitivity to autologous plasma in contrast to other autologous Envs obtained at the same time point. By constructing chimeric Envs and fine mapping between sensitive and resistant Env clones, we found that substitution of highly conserved isoleucine (I) with methionine (M) (ATA to ATG) at position 424 in the C4 domain conferred enhanced neutralization sensitivity of Env-pseudotyped viruses to autologous and heterologous plasma antibodies. When tested against monoclonal antibodies targeting different sites in gp120 and gp41, Envs expressing M424 showed significant sensitivity to anti-V3 monoclonal antibodies and modestly to sCD4 and b12. Substitution of I424M in unrelated Envs also showed similar neutralization phenotype, indicating that M424 in C4 region induces exposure of neutralizing epitopes particularly in CD4 binding sites and V3 loop.
摘要
鉴定 HIV-1 包膜(Env)的弱点将有助于基于 Env 的疫苗设计。我们最近从一名最近感染的印度患者中扩增出了一株 HIV-1 克隆 C Env 克隆(4-2.J45),与同时获得的其他自体 Env 相比,该克隆对自体血浆具有异常的中和敏感性。通过构建嵌合 Env,并在敏感和耐药 Env 克隆之间进行精细定位,我们发现 C4 结构域中位置 424 的高度保守异亮氨酸(I)突变为蛋氨酸(M)(ATA 突变为 ATG),可增强 Env 假型病毒对自体和异体血浆抗体的中和敏感性。当用针对 gp120 和 gp41 不同位点的单克隆抗体进行测试时,表达 M424 的 Envs 对抗 V3 单克隆抗体表现出显著的敏感性,对 sCD4 和 b12 的敏感性适度。在不相关的 Env 中替换 I424M 也显示出类似的中和表型,表明 C4 区域中的 M424 诱导中和表位的暴露,特别是在 CD4 结合位点和 V3 环中。
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