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Research Article

Vaccination with a synthetic peptide from the influenza virus hemagglutinin provides protection against distinct viral subtypes

Taia T. Wang, Gene S. Tan, Rong Hai, Natalie Pica, Lily Ngai, Damian C. Ekiert, Ian A. Wilson, Adolfo García-Sastre, Thomas M. Moran, and Peter Palese
  1. Departments of aMicrobiology and
  2. dMedicine,
  3. eEmerging Pathogens Institute, and
  4. fImmunology Institute, Mount Sinai School of Medicine, New York, NY 10029; and
  5. bDepartment of Molecular Biology and
  6. cSkaggs Institute for Chemical Biology, The Scripps Research Institute, La Jolla, CA 92037

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PNAS first published October 18, 2010; https://doi.org/10.1073/pnas.1013387107
Taia T. Wang
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Gene S. Tan
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Rong Hai
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Natalie Pica
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Lily Ngai
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Damian C. Ekiert
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Ian A. Wilson
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Adolfo García-Sastre
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Thomas M. Moran
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Peter Palese
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  • For correspondence: peter.palese@mssm.edu
  1. Contributed by Peter Palese, September 10, 2010 (sent for review August 25, 2010)

  2. ↵1T.T.W. and G.S.T. contributed equally to this work.

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Abstract

Current influenza virus vaccines protect mostly against homologous virus strains; thus, regular immunization with updated vaccine formulations is necessary to guard against the virus' hallmark remodeling of regions that mediate neutralization. Development of a broadly protective influenza vaccine would mark a significant advance in human infectious diseases research. Antibodies with broad neutralizing activity (nAbs) against multiple influenza virus strains or subtypes have been reported to bind the stalk of the viral hemagglutinin, suggesting that a vaccine based on this region could elicit a broadly protective immune response. Here we describe a hemagglutinin subunit 2 protein (HA2)-based synthetic peptide vaccine that provides protection in mice against influenza viruses of the structurally divergent subtypes H3N2, H1N1, and H5N1. The immunogen is based on the binding site of the recently described nAb 12D1, which neutralizes H3 subtype viruses, demonstrates protective activity in vivo, and, in contrast to a majority of described nAbs, appears to bind to residues within a single α-helical portion of the HA2 protein. Our data further demonstrate that the specific design of our immunogen is integral in the induction of broadly active anti-hemagglutinin antibodies. These results provide proof of concept for an HA2-based influenza vaccine that could diminish the threat of pandemic influenza disease and generally reduce the significance of influenza viruses as human pathogens.

  • mice
  • pandemic
  • synthetic peptide
  • vaccine
  • HA2

Footnotes

  • 2To whom correspondence should be addressed. E-mail: peter.palese{at}mssm.edu.
  • Author contributions: T.T.W., G.S.T., D.C.E., I.A.W., A.G.-S., T.M.M., and P.P. designed research; T.T.W., G.S.T., R.H., N.P., L.N., and D.C.E. performed research; T.T.W., G.S.T., and P.P. analyzed data; and T.T.W. and P.P. wrote the paper.

  • Conflict of interest statement: Mount Sinai School of Medicine has filed a provisional patent covering some of the results described in this paper.

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Vaccination with a synthetic peptide from the influenza virus hemagglutinin provides protection against distinct viral subtypes
Taia T. Wang, Gene S. Tan, Rong Hai, Natalie Pica, Lily Ngai, Damian C. Ekiert, Ian A. Wilson, Adolfo García-Sastre, Thomas M. Moran, Peter Palese
Proceedings of the National Academy of Sciences Oct 2010, 201013387; DOI: 10.1073/pnas.1013387107

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Vaccination with a synthetic peptide from the influenza virus hemagglutinin provides protection against distinct viral subtypes
Taia T. Wang, Gene S. Tan, Rong Hai, Natalie Pica, Lily Ngai, Damian C. Ekiert, Ian A. Wilson, Adolfo García-Sastre, Thomas M. Moran, Peter Palese
Proceedings of the National Academy of Sciences Oct 2010, 201013387; DOI: 10.1073/pnas.1013387107
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