首页> 美国卫生研究院文献>Journal of Virology >Neutralization Efficiency Is Greatly Enhanced by Bivalent Binding of an Antibody to Epitopes in the V4 Region and the Membrane-Proximal External Region within One Trimer of Human Immunodeficiency Virus Type 1 Glycoproteins
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Neutralization Efficiency Is Greatly Enhanced by Bivalent Binding of an Antibody to Epitopes in the V4 Region and the Membrane-Proximal External Region within One Trimer of Human Immunodeficiency Virus Type 1 Glycoproteins

机译:通过将抗体与人免疫缺陷病毒1型糖蛋白的一个三聚体中的V4区和膜近端外部区的表位二价结合可大大提高中和效率。

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摘要

Most antibodies are multivalent, with the potential to bind with high avidity. However, neutralizing antibodies commonly bind to virions monovalently. Bivalent binding of a monoclonal antibody (MAb) to a virion has been documented only in a single case. Thus, the role of high avidity in antibody-mediated neutralization of viruses has not been defined clearly. In this study, we demonstrated that when an artificial 2F5 epitope was inserted in the gp120 V4 region so that an HIV-1 envelope glycoprotein (Env) trimer contains a natural 2F5 epitope in the gp41 membrane-proximal envelope region (MPER) and an artificially engineered 2F5 epitope in the gp120 V4 region, bivalent 2F5 IgG achieved greatly enhanced neutralization efficiency, with a 50% inhibitory concentration (IC50) decrease over a 2-log scale. In contrast, the monovalent 2F5 Fab fragment did not exhibit any appreciable change in neutralization efficiency in the same context. These results demonstrate that bivalent binding of 2F5 IgG to a single HIV-1 Env trimer results in dramatic enhancement of neutralization, probably through an increase in binding avidity. Furthermore, we demonstrated that bivalent binding of MAb 2F5 to the V4 region and MPER of an HIV-1 Env trimer can be achieved only in a specific configuration, providing an important insight into the structure of a native/infectious HIV-1 Env trimer. This specific binding configuration also establishes a useful standard that can be applied to evaluate the biological relevance of structural information on the HIV-1 Env trimer.
机译:大多数抗体是多价的,具有高亲和力结合的潜力。然而,中和抗体通常单价结合病毒体。单克隆抗体(MAb)与病毒体的二价结合仅在单个案例中有文献记载。因此,尚不清楚高亲和力在抗体介导的病毒中和中的作用。在这项研究中,我们证明了当在gp120 V4区域中插入人工2F5表位时,HIV-1包膜糖蛋白(Env)三聚体在gp41膜近端包膜区域(MPER)中包含一个天然2F5表位,在gp120 V4区域设计了2F5表位,二价2F5 IgG大大提高了中和效率,抑制浓度(IC50)降低了2个对数级。相反,在相同情况下,单价2F5 Fab片段在中和效率方面没有表现出任何明显的变化。这些结果表明,2F5 IgG与单个HIV-1 Env三聚体的二价结合可能显着增强中和作用,可能是通过增加结合亲和力来实现的。此外,我们证明,MAb 2F5与HIV-1 Env三聚体的V4区和MPER的二价结合只能在特定的配置下实现,从而提供了对天然/感染性HIV-1 Env三聚体结构的重要认识。这种特异性结合构型还建立了有用的标准,可用于评估HIV-1 Env三聚体上结构信息的生物学相关性。

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