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奥密克戎对抗体中和作用的逃逸显著。

Considerable escape of SARS-CoV-2 Omicron to antibody neutralization.

机构信息

Virus and Immunity Unit, Institut Pasteur, Université de Paris, CNRS UMR3569, Paris, France.

Vaccine Research Institute, Créteil, France.

出版信息

Nature. 2022 Feb;602(7898):671-675. doi: 10.1038/s41586-021-04389-z. Epub 2021 Dec 23.

Abstract

The SARS-CoV-2 Omicron variant was first identified in November 2021 in Botswana and South Africa. It has since spread to many countries and is expected to rapidly become dominant worldwide. The lineage is characterized by the presence of around 32 mutations in spike-located mostly in the N-terminal domain and the receptor-binding domain-that may enhance viral fitness and enable antibody evasion. Here we isolated an infectious Omicron virus in Belgium from a traveller returning from Egypt. We examined its sensitivity to nine monoclonal antibodies that have been clinically approved or are in development, and to antibodies present in 115 serum samples from COVID-19 vaccine recipients or individuals who have recovered from COVID-19. Omicron was completely or partially resistant to neutralization by all monoclonal antibodies tested. Sera from recipients of the Pfizer or AstraZeneca vaccine, sampled five months after complete vaccination, barely inhibited Omicron. Sera from COVID-19-convalescent patients collected 6 or 12 months after symptoms displayed low or no neutralizing activity against Omicron. Administration of a booster Pfizer dose as well as vaccination of previously infected individuals generated an anti-Omicron neutralizing response, with titres 6-fold to 23-fold lower against Omicron compared with those against Delta. Thus, Omicron escapes most therapeutic monoclonal antibodies and, to a large extent, vaccine-elicited antibodies. However, Omicron is neutralized by antibodies generated by a booster vaccine dose.

摘要

SARS-CoV-2 奥密克戎变异株于 2021 年 11 月在博茨瓦纳和南非首次被发现。自那时以来,它已传播到许多国家,预计将在全球迅速成为主要流行株。该谱系的特征是棘突蛋白上存在约 32 个突变,主要位于 N 端结构域和受体结合域,这可能增强病毒适应性并使抗体逃逸。在这里,我们从一名从埃及返回的旅行者身上分离出比利时的传染性奥密克戎病毒。我们研究了它对 9 种已获得临床批准或正在开发的单克隆抗体以及 115 份来自 COVID-19 疫苗接种者或从 COVID-19 中康复的个体血清样本中存在的抗体的敏感性。奥密克戎对所有测试的单克隆抗体完全或部分具有抗中和作用。在完全接种疫苗五个月后采集的辉瑞或阿斯利康疫苗接种者的血清几乎不能抑制奥密克戎。在出现症状 6 或 12 个月后采集的 COVID-19 康复患者的血清对奥密克戎的中和活性较低或没有。接种辉瑞加强剂量以及接种以前感染过的个体可产生针对奥密克戎的中和反应,与针对德尔塔的滴度相比,针对奥密克戎的滴度降低了 6 至 23 倍。因此,奥密克戎逃避了大多数治疗性单克隆抗体,并且在很大程度上逃避了疫苗诱导的抗体。然而,奥密克戎被加强疫苗剂量产生的抗体中和。

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