501Y.V2 and 501Y.V3 variants of SARS-CoV-2 lose binding to Bamlanivimab in vitro

Haolin Liu,Peng Cheng-wei,Qianqian Zhang,Zhongzhou Chen,Katja Aviszus,Walter Downing,Shelley Peterson,Lyndon Reynoso,Gregory P. Downey,Stephen K. Frankel,John W. Kappler,Philippa Marrack,Gongyi Zhang

501Y.V2 and 501Y.V3 variants of SARS-CoV-2 lose binding to Bamlanivimab in vitro

2021

Haolin Liu
Peng Cheng-wei
Qianqian Zhang
Zhongzhou Chen
Katja Aviszus
Walter Downing
Shelley Peterson
Lyndon Reynoso
Gregory P. Downey
Stephen K. Frankel
John W. Kappler
Philippa Marrack
Gongyi Zhang

We generated several versions of the receptor binding domain (RBD) of the Spike protein with mutations existing within newly emerging variants from South Africa and Brazil. We found that the mutant RBD with K417N, E484K, and N501Y exchanges has higher binding affinity to the human receptor compared to the wildtype RBD. This mutated version of RBD also completely abolishes the binding to a therapeutic antibody, Bamlanivimab, in vitro .

Keywords:

Wild type
severe acute respiratory syndrome coronavirus 2
In vitro
Ligand (biochemistry)
Virology
Spike Protein
Biology
therapeutic antibody
Receptor
Mutant

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations