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A SARS-CoV-2 neutralizing antibody selected from COVID-19 patients binds to the ACE2-RBD interface and is tolerant to most known RBD mutations

机译:选自Covid-19患者的SARS-COV-2中和抗体与ACE2-RBD界面结合,耐受最着名的RBD突变

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摘要

The novel betacoronavirus severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2) causes a form of severe pneumonia disease called coronavirus disease 2019 (COVID-19). To develop human neutralizing anti-SARS-CoV-2 antibodies, antibody gene libraries from convalescent COVID-19 patients were constructed and recombinant antibody fragments (scFv) against the receptor-binding domain (RBD) of the spike protein were selected by phage display. The antibody STE90-C11 shows a subnanometer IC 50 in a plaque-based live SARS-CoV-2 neutralization assay. The in?vivo efficacy of the antibody is demonstrated in the Syrian hamster and in the human angiotensin-converting enzyme 2 (hACE2) mice model. The crystal structure of STE90-C11 Fab in complex with SARS-CoV-2-RBD is solved at 2.0?? resolution showing that the antibody binds at the same region as ACE2 to RBD. The binding and inhibition of STE90-C11 is not blocked by many known emerging RBD mutations. STE90-C11-derived human IgG1 with FcγR-silenced Fc (COR-101) is undergoing Phase Ib/II clinical trials for the treatment of moderate to severe COVID-19.
机译:新型的βAvoronavirus重度急性呼吸综合征 - 冠状病毒-2(SARS-COV-2)导致一种叫做冠状病毒疾病2019(Covid-19)的严重肺炎病的形式。为了开发人中和抗SARS-COV-2抗体,通过噬菌体展示来构建来自临床Covid-19患者的抗体基因文库,并通过噬菌体展示选择刺激蛋白的受体结合结构域(RBD)的重组抗体片段(SCFV)。抗体STE90-C11在基于斑块的活SARS-COV-2中和中和测定中示出了亚域IC 50。在叙利亚仓鼠和人血管紧张素转换酶2(Hace2)小鼠模型中证明了抗体的体内疗效。与SARS-COV-2-RBD复合物的STE90-C11 Fab的晶体结构在2.0 ??分辨率表明抗体在与ACE2相同的区域与RBD结合。 STE90-C11的结合和抑制不受许多已知的新一种RBD突变阻断。 STE90-C11衍生的人IgG1与FCγR沉默的Fc(Cor-101)正在进行IB / II期临床试验,用于治疗中度至重度Covid-19。

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