Affinity Maturation Endows Potent Activity Onto Class 6 SARS-CoV-2 Broadly Neutralizing Antibodies

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2025 Jan 2

PMID 39746041

Authors

Ohan Mazigi

David B Langley

Jake Y Henry

Deborah L Burnett

Meghna Sobti

Gregory J Walker

Romain Rouet

Harikrishnan Balachandran

Helen Lenthall

Jennifer Jackson

Stephanie Ubiparipovic

Peter Schofield

Simon H J Brown

Sebastian R Schulz

Markus Hoffmann

Stefan Pohlmann

Jeffrey Post

Marianne Martinello

Golo Ahlenstiel

Anthony Kelleher

William D Rawlinson

Stuart G Turville

Rowena A Bull

Alastair G Stewart

Hans-Martin Jack

Christopher C Goodnow

Daniel Christ

Affiliations

Soon will be listed here.

Abstract

The emergence of SARS-CoV-2 variants of concern (VOCs) has greatly diminished the neutralizing activity of previously FDA-approved monoclonal antibodies (mAbs), including that of antibody cocktails and of first-generation broadly neutralizing antibodies such as S309 (Sotrovimab). In contrast, antibodies targeting cryptic conformational epitopes of the receptor binding domain (RBD) have demonstrated broad activity against emerging variants, but exert only moderate neutralizing activity, which has so far hindered clinical development. Here, we utilize in vitro display technology to identify and affinity-mature antibodies targeting the cryptic class 6 epitope, accessible only in the "up" conformation of the SARS-CoV-2 spike trimer. Increasing antibody affinity into the low picomolar range endowed potent neutralization of VOCs and protection of hACE2 mice from viral challenge. Cryoelectron microscopy and crystal structures of two affinity-matured antibodies (4C12-B12 and 4G1-C2) in complex with RBD highlighted binding modes and epitopes distal from mutational hotspots commonly overserved in VOCs, providing direct structural insights into the observed mutational resistance. Moreover, we further demonstrate that antibodies targeting the class 6 epitope, rather than being an artifact of in vitro selection, are common in the IgG1 memory B cell repertoire of convalescent patients and can be induced in human antibody V-gene transgenic mice through immunization. Our results highlight the importance of very high (picomolar) affinity in the development of neutralizing antibodies and vaccines and suggest an affinity threshold in the provision of broad and long-lasting immunity against SARS-CoV-2.

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