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Immunizations with diverse sarbecovirus receptor-binding domains elicit SARS-CoV-2 neutralizing antibodies against a conserved site of vulnerability

Immunity. 2021-10; 
Deborah L Burnett, Katherine J L Jackson, David B Langley, Anupria Aggrawal, Alberto Ospina Stella, Matt D Johansen, Harikrishnan Balachandran, Helen Lenthall, Romain Rouet, Gregory Walker, Bernadette M Saunders, Mandeep Singh, Hui Li, Jake Y Henry, Jennifer Jackson, Alastair G Stewart, Franka Witthauer, Matthew A Spence, Nicole G Hansbro, Colin Jackson, Peter Schofield, Claire Milthorpe, Marianne Martinello, Sebastian R Schulz, Edith Roth, Anthony Kelleher, Sean Emery, Warwick J Britton, William D Rawlinson, Rudolfo Karl, Simon Sch?fer, Thomas H Winkler, Robert Brink, Rowena A Bull, Philip M Hansbro, Hans-Martin J?ck, Stuart Turville, Daniel Christ, Christopher C Goodnow
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摘要

Viral mutations are an emerging concern in reducing SARS-CoV-2 vaccination efficacy. Second-generation vaccines will need to elicit neutralizing antibodies against sites that are evolutionarily conserved across the sarbecovirus subgenus. Here, we immunized mice containing a human antibody repertoire with diverse sarbecovirus receptor-binding domains (RBDs) to identify antibodies targeting conserved sites of vulnerability. Antibodies with broad reactivity against diverse clade B RBDs targeting the conserved class 4 epitope, with recurring IGHV/IGKV pairs, were readily elicited but were non-neutralizing. However, rare class 4 antibodies binding this conserved RBD supersite showed potent neutralization of SARS-CoV... More

關鍵詞

SARS-CoV-2, antigenic variation, class 4 epitope site, cross-reactivity, epitope conservation, escape mutations, human antibodies, mouse model, neutralization, next generation vaccines, variants of concern
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