Monoclonal antibodies directed against trimeric forms of the HIV-1 envelope glycoprotein with broad and potent neutralizing activity

Assignees

• International AIDS Vaccine Initiative, Inc. · US
• THE SCRIPPS RESEARCH INSTITUTE · US
• Theraclone Sciences Inc. · US

Inventors

• Po-Ying Chan-Hui · Bellevue, US
• Steven Frey · Redmond, US
• Ole Olsen · Everett, US
• Jennifer Mitcham · Redmond, US
• Matthew Moyle · Redmond, US
• Sanjay K. Phogat · Frederick, US
• Dennis R. Burton · Village of La Jolla, US
• Laura Marjorie Walker · San Diego, US
• Pascal Raymond Georges Poignard · San Diego, US
• Wayne Koff · Stony Brook, US
• Melissa Danielle De Jean De St. Marcel Simek-Lemos · Brooklyn, US
• Stephen Kaminsky · The Bronx, US

Key dates

Classification

• Technology area (CPC C)Chemistry; Metallurgy
• CPC primaryC07K2317/76
• WIPO fieldPharmaceuticals
• WIPO sectorChemistry

Abstract

The invention provides a method for obtaining a broadly neutralizing antibody (bNab), including screening memory B cell cultures from a donor PBMC sample for neutralization activity against a plurality of HIV-1 species, cloning a memory B cell that exhibits broad neutralization activity; and rescuing a monoclonal antibody from that memory B cell culture. The resultant monoclonal antibodies are characterized by their ability to selectively bind epitopes from the Env proteins in native or monomeric form, as well as to inhibit infection of HIV-1 species from a plurality of clades. Compositions containing human monoclonal anti-HIV antibodies used for prophylaxis, diagnosis and treatment of HIV infection are provided. Methods for generating such antibodies by immunization using epitopes from conserved regions within the variable loops of gp120 are provided. Immunogens for generating anti-HIV1 bNAbs are also provided. Furthermore, methods for vaccination using suitable epitopes are provided.