Pentavalent HIV-1 vaccine protects against simian-human immunodeficiency virus challenge

نویسندگان

  • Todd Bradley
  • Justin Pollara
  • Sampa Santra
  • Nathan Vandergrift
  • Srivamshi Pittala
  • Chris Bailey-Kellogg
  • Xiaoying Shen
  • Robert Parks
  • Derrick Goodman
  • Amanda Eaton
  • Harikrishnan Balachandran
  • Linh V. Mach
  • Kevin O. Saunders
  • Joshua A. Weiner
  • Richard Scearce
  • Laura L. Sutherland
  • Sanjay Phogat
  • Jim Tartaglia
  • Steven G. Reed
  • Shiu-Lok Hu
  • James F. Theis
  • Abraham Pinter
  • David C. Montefiori
  • Thomas B. Kepler
  • Kristina K. Peachman
  • Mangala Rao
  • Nelson L. Michael
  • Todd J. Suscovich
  • Galit Alter
  • Margaret E. Ackerman
  • M. Anthony Moody
  • Hua-Xin Liao
  • Georgia Tomaras
  • Guido Ferrari
  • Bette T. Korber
  • Barton F. Haynes
چکیده

The RV144 Thai trial HIV-1 vaccine of recombinant poxvirus (ALVAC) and recombinant HIV-1 gp120 subtype B/subtype E (B/E) proteins demonstrated 31% vaccine efficacy. Here we design an ALVAC/Pentavalent B/E/E/E/E vaccine to increase the diversity of gp120 motifs in the immunogen to elicit a broader antibody response and enhance protection. We find that immunization of rhesus macaques with the pentavalent vaccine results in protection of 55% of pentavalent-vaccine-immunized macaques from simian-human immunodeficiency virus (SHIV) challenge. Systems serology of the antibody responses identifies plasma antibody binding to HIV-infected cells, peak ADCC antibody titres, NK cell-mediated ADCC and antibody-mediated activation of MIP-1β in NK cells as the four immunological parameters that best predict decreased infection risk that are improved by the pentavalent vaccine. Thus inclusion of additional gp120 immunogens to a pox-prime/protein boost regimen can augment antibody responses and enhance protection from a SHIV challenge in rhesus macaques.

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عنوان ژورنال:

دوره 8  شماره 

صفحات  -

تاریخ انتشار 2017