Liu Haolin, Zhang Qianqian, Wei Pengcheng, Chen Zhongzhou, Aviszus Katja, Yang John, Downing Walter, Peterson Shelley, Jiang Chengyu, Liang Bo, Reynoso Lyndon, Downey Gregory P, Frankel Stephen K, Kappler John, Marrack Philippa, Zhang Gongyi
bioRxiv. 2021 Feb 2:2021.02.02.428884. doi: 10.1101/2021.02.02.428884.
Severe acute respiratory syndrome-related coronavirus 2 (SARS-CoV-2) is causing a world-wide pandemic. A variant of SARS-COV-2 (20I/501Y.V1) recently discovered in the United Kingdom has a single mutation from N501 to Y501 within the receptor binding domain (Y501-RBD), of the Spike protein of the virus. This variant is much more contagious than the original version (N501-RBD). We found that this mutated version of RBD binds to human Angiotensin Converting Enzyme 2 (ACE2) a ~10 times more tightly than the native version (N501-RBD). Modeling analysis showed that the N501Y mutation would allow a potential aromatic ring-ring interaction and an additional hydrogen bond between the RBD and ACE2. However, sera from individuals immunized with the Pfizer-BioNTech vaccine still efficiently block the binding of Y501-RBD to ACE2 though with a slight compromised manner by comparison with their ability to inhibit binding to ACE2 of N501-RBD. This may raise the concern whether therapeutic anti-RBD antibodies used to treat COVID-19 patients are still efficacious. Nevertheless, a therapeutic antibody, Bamlanivimab, still binds to the Y501-RBD as efficiently as its binds to N501-RBD.
严重急性呼吸综合征相关冠状病毒2(SARS-CoV-2)正在引发全球大流行。最近在英国发现的一种SARS-CoV-2变体(20I/501Y.V1)在病毒刺突蛋白的受体结合域(Y501-RBD)内有一个从N501到Y501的单突变。这种变体比原始版本(N501-RBD)更具传染性。我们发现,这种突变版本的RBD与人血管紧张素转换酶2(ACE2)的结合比天然版本(N501-RBD)紧密约10倍。建模分析表明,N501Y突变将允许RBD与ACE2之间形成潜在的芳香环-环相互作用和额外的氢键。然而,接种辉瑞-BioNTech疫苗的个体的血清仍然能够有效地阻断Y501-RBD与ACE2的结合,尽管与它们抑制N501-RBD与ACE2结合的能力相比略有下降。这可能会引发人们对用于治疗COVID-19患者的治疗性抗RBD抗体是否仍然有效的担忧。尽管如此,一种治疗性抗体巴姆兰尼单抗(Bamlanivimab)与Y501-RBD的结合效率仍与其与N501-RBD的结合效率相同。
