Antibody-directed evolution reveals a mechanism for enhanced neutralization at the HIV-1 fusion peptide site

Author:

Banach Bailey B.,Pletnev Sergei,Olia Adam S.,Xu Kai,Zhang Baoshan,Rawi RedaORCID,Bylund Tatsiana,Doria-Rose Nicole A.ORCID,Nguyen Thuy Duong,Fahad Ahmed S.,Lee MyungjinORCID,Lin Bob C.,Liu Tracy,Louder Mark K.ORCID,Madan Bharat,McKee Krisha,O’Dell Sijy,Sastry Mallika,Schön Arne,Bui Natalie,Shen Chen-Hsiang,Wolfe Jacy R.,Chuang Gwo-Yu,Mascola John R.,Kwong Peter D.ORCID,DeKosky Brandon J.ORCID

Abstract

AbstractThe HIV-1 fusion peptide (FP) represents a promising vaccine target, but global FP sequence diversity among circulating strains has limited anti-FP antibodies to ~60% neutralization breadth. Here we evolve the FP-targeting antibody VRC34.01 in vitro to enhance FP-neutralization using site saturation mutagenesis and yeast display. Successive rounds of directed evolution by iterative selection of antibodies for binding to resistant HIV-1 strains establish a variant, VRC34.01_mm28, as a best-in-class antibody with 10-fold enhanced potency compared to the template antibody and ~80% breadth on a cross-clade 208-strain neutralization panel. Structural analyses demonstrate that the improved paratope expands the FP binding groove to accommodate diverse FP sequences of different lengths while also recognizing the HIV-1 Env backbone. These data reveal critical antibody features for enhanced neutralization breadth and potency against the FP site of vulnerability and accelerate clinical development of broad HIV-1 FP-targeting vaccines and therapeutics.

Funder

U.S. Department of Health & Human Services | NIH | National Cancer Institute

U.S. Department of Health & Human Services | National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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