A Highly Conserved Neutralizing Epitope on Group 2 Influenza A Viruses

Damian C. Ekiert(Scripps Research Institute), Robert H. Friesen(Johnson & Johnson (Netherlands)), Gira Bhabha(Scripps Research Institute), Ted Kwaks(Johnson & Johnson (Netherlands)), Mandy Jongeneelen(Johnson & Johnson (Netherlands)), Wenli Yu(Scripps Research Institute), C. Ophorst(Johnson & Johnson (Netherlands)), Freek Cox(Johnson & Johnson (Netherlands)), Hans J. W. M. Korse(Johnson & Johnson (Netherlands)), Boerries Brandenburg(Johnson & Johnson (Netherlands)), Ronald Vogels(Johnson & Johnson (Netherlands)), Just P. J. Brakenhoff(Johnson & Johnson (Netherlands)), Ronald Kompier(Johnson & Johnson (Netherlands)), Martin H. Koldijk(Johnson & Johnson (Netherlands)), Lisette A. H. M. Cornelissen(Wageningen University & Research), Leo L. M. Poon(University of Hong Kong), Malik Peiris(University of Hong Kong), Wouter Koudstaal(Johnson & Johnson (Netherlands)), Ian A. Wilson(Scripps Research Institute), Jaap Goudsmit(Johnson & Johnson (Netherlands))
Science
July 8, 2011
10.1126/science.1204839
Cited by 858

Abstract

Current flu vaccines provide only limited coverage against seasonal strains of influenza viruses. The identification of V(H)1-69 antibodies that broadly neutralize almost all influenza A group 1 viruses constituted a breakthrough in the influenza field. Here, we report the isolation and characterization of a human monoclonal antibody CR8020 with broad neutralizing activity against most group 2 viruses, including H3N2 and H7N7, which cause severe human infection. The crystal structure of Fab CR8020 with the 1968 pandemic H3 hemagglutinin (HA) reveals a highly conserved epitope in the HA stalk distinct from the epitope recognized by the V(H)1-69 group 1 antibodies. Thus, a cocktail of two antibodies may be sufficient to neutralize most influenza A subtypes and, hence, enable development of a universal flu vaccine and broad-spectrum antibody therapies.

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