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Comprehensive Mapping of HIV-1 Escape from a Broadly Neutralizing Antibody

机译:HIV-1的综合映射从广泛中和抗体逃脱

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Precisely defining how viral mutations affect HIV's sensitivity to antibodies is vital to develop and evaluate vaccines and antibody immunotherapeutics. Despite great effort, a full map of escape mutants has not been delineated for an anti-HIV antibody. We describe a massively parallel experimental approach to quantify how all single amino acid mutations to HIV Envelope (Env) affect neutralizing antibody sensitivity in the context of replication-competent virus. We apply this approach to PGT151, a broadly neutralizing antibody recognizing a combination of Env residues and glycans. We confirm sites previously defined by structural and functional studies and reveal additional sites of escape, such as positively charged mutations in the antibody-Env interface. Evaluating the effect of each amino acid at each site lends insight into biochemical mechanisms of escape throughout the epitope, highlighting roles for charge-charge repulsions. Thus, comprehensively mapping HIV antibody escape gives a quantitative, mutation-level view of Env evasion of neutralization.
机译:精确地定义病毒突变如何影响艾滋病毒对抗体的敏感性至关重要,可发展和评估疫苗和抗体免疫治疗。尽管努力,但抗HIV抗体尚未划算逃生突变体的完整地图。我们描述了一种大规模平行的实验方法来量化所有单个氨基酸突变到HIV封套(ENV)如何影响复制态病毒的背景下的中和抗体敏感性。我们将这种方法应用于PGT151,这是一种概括苯残基和聚糖组合的宽度中和抗体。我们确认先前由结构和功能研究定义的网站,并揭示额外的逃生部位,例如抗体 - ENV界面中的带正电荷突变。评估每个位点的每种氨基酸的效果倾向于在整个表位的逃逸的生化机制中,突出占电荷排斥的作用。因此,综合定位HIV抗体逃逸给出了env逃避中和的定量突变水平视图。

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