| Literature DB >> 24335589 |
Robert H E Friesen1, Peter S Lee, Esther J M Stoop, Ryan M B Hoffman, Damian C Ekiert, Gira Bhabha, Wenli Yu, Jarek Juraszek, Wouter Koudstaal, Mandy Jongeneelen, Hans J W M Korse, Carla Ophorst, Els C M Brinkman-van der Linden, Mark Throsby, Mark J Kwakkenbos, Arjen Q Bakker, Tim Beaumont, Hergen Spits, Ted Kwaks, Ronald Vogels, Andrew B Ward, Jaap Goudsmit, Ian A Wilson.
Abstract
The discovery and characterization of broadly neutralizing antibodies (bnAbs) against influenza viruses have raised hopes for the development of monoclonal antibody (mAb)-based immunotherapy and the design of universal influenza vaccines. Only one human bnAb (CR8020) specifically recognizing group 2 influenza A viruses has been previously characterized that binds to a highly conserved epitope at the base of the hemagglutinin (HA) stem and has neutralizing activity against H3, H7, and H10 viruses. Here, we report a second group 2 bnAb, CR8043, which was derived from a different germ-line gene encoding a highly divergent amino acid sequence. CR8043 has in vitro neutralizing activity against H3 and H10 viruses and protects mice against challenge with a lethal dose of H3N2 and H7N7 viruses. The crystal structure and EM reconstructions of the CR8043-H3 HA complex revealed that CR8043 binds to a site similar to the CR8020 epitope but uses an alternative angle of approach and a distinct set of interactions. The identification of another antibody against the group 2 stem epitope suggests that this conserved site of vulnerability has great potential for design of therapeutics and vaccines.Entities:
Keywords: X-ray crystallography; antibody recognition; electron microscopy
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Year: 2013 PMID: 24335589 PMCID: PMC3890827 DOI: 10.1073/pnas.1319058110
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205