| Literature DB >> 34074219 |
Haolin Liu1,2, Pengcheng Wei1,2, Qianqian Zhang3, Zhongzhou Chen3, Katja Aviszus1,2, Walter Downing4, Shelley Peterson4, Lyndon Reynoso5, Gregory P Downey6, Stephen K Frankel6, John Kappler1,2, Philippa Marrack1,2, Gongyi Zhang1,2.
Abstract
The newly emerging variants of SARS-CoV-2 from South Africa (B.1.351/501Y.V2) and Brazil (P.1/501Y.V3) have led to a higher infection rate and reinfection of COVID-19 patients. We found that the mutations K417N, E484K, and N501Y within the receptor-binding domains (RBDs) of the virus could confer ~2-fold higher binding affinity to the human receptor, angiotensin converting enzyme 2 (ACE2), compared to the wildtype RBD. The mutated version of RBD also completely abolishes the binding of bamlanivimab, a therapeutic antibody, in vitro. Detailed analysis shows that the ~10-fold gain of binding affinity between ACE2 and Y501-RBD, which also exits in the high contagious variant B.1.1.7/501Y.V1 from the United Kingdom, is compromised by additional introduction of the K417/N/T mutation. Mutation of E484K leads to the loss of bamlanivimab binding to RBD, although this mutation does not affect the binding between RBD and ACE2.Entities:
Keywords: ACE2; B.1.1.7/501Y.V1; B.1.351/501Y.V2; COVID-19; P.1/501Y.V3; RBD; Bamlanivimab; SARS-COV-2
Year: 2021 PMID: 34074219 DOI: 10.1080/19420862.2021.1919285
Source DB: PubMed Journal: MAbs ISSN: 1942-0862 Impact factor: 5.857