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Structural Basis for a Neutralizing Antibody Response Elicited by a Recombinant Hantaan Virus Gn Immunogen

机译:通过重组汉坦病毒GN免疫原引发中和抗体应答的结构基础

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ABSTRACT Hantaviruses are a group of emerging pathogens capable of causing severe disease upon zoonotic transmission to humans. The mature hantavirus surface presents higher-order tetrameric assemblies of two glycoproteins, Gn and Gc, which are responsible for negotiating host cell entry and constitute key therapeutic targets. Here, we demonstrate that recombinantly derived Gn from Hantaan virus (HTNV) elicits a neutralizing antibody response (serum dilution that inhibits 50% infection [ID _(50)], 1:200 to 1:850) in an animal model. Using antigen-specific B cell sorting, we isolated monoclonal antibodies (mAbs) exhibiting neutralizing and non-neutralizing activity, termed mAb HTN-Gn1 and mAb nnHTN-Gn2, respectively. Crystallographic analysis reveals that these mAbs target spatially distinct epitopes at disparate sites of the N-terminal region of the HTNV Gn ectodomain. Epitope mapping onto a model of the higher order (Gn-Gc) _(4) spike supports the immune accessibility of the mAb HTN-Gn1 epitope, a hypothesis confirmed by electron cryo-tomography of the antibody with virus-like particles. These data define natively exposed regions of the hantaviral Gn that can be targeted in immunogen design.
机译:摘要Hantaviruses是一群能够在对人类传播中引起严重疾病的新兴病原体。成熟的Hantavirus表面呈现出两种糖蛋白,GN和GC的高阶四聚体组件,其负责促进宿主细胞进入并构成关键治疗靶标。在这里,我们证明了来自汉丹病毒(HTNV)的重组衍生的GN引发了中和抗体反应(血清稀释,抑制动物模型中的50%感染[ID _(50)],1:200至1:850)。使用特异性B细胞分选,我们分离出表现出中和和非中和活性的单克隆抗体(MAB),分别称为MAB HTN-GN1和MAB NNHTN-GN2。结晶分析表明,这些MAB在HTNV GN胞菌素的N-末端区域的不同位点靶出空间上不同的表位。表位映射到更高阶(GN-GC)_(4)秒的模型上,支持MAB HTN-GN1表位的免疫可接触性,该假设通过抗体的电子粘度术与病毒样颗粒进行了证实。这些数据定义了本地暴露于可以靶向免疫原设计的汉语血岭GN的区域。

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