Immunogenicity and efficacy of flagellin-envelope fusion dengue vaccines in mice and monkeys.

نویسندگان

  • Ge Liu
  • Langzhou Song
  • David W C Beasley
  • Robert Putnak
  • Jason Parent
  • John Misczak
  • Hong Li
  • Lucia Reiserova
  • Xiangyu Liu
  • Haijun Tian
  • Wenzhe Liu
  • Darlene Labonte
  • Lihua Duan
  • Youngsun Kim
  • Linda Travalent
  • Devin Wigington
  • Bruce Weaver
  • Lynda Tussey
چکیده

The envelope (E) protein of flaviviruses includes three domains, EI, EII, and EIII, and is the major protective antigen. Because EIII is rich in type-specific and subcomplex-specific neutralizing epitopes and is easy to express, it is particularly attractive as a recombinant vaccine antigen. VaxInnate has developed a vaccine platform that genetically links vaccine antigens to bacterial flagellin, a Toll-like receptor 5 ligand. Here we report that tetravalent dengue vaccines (TDVs) consisting of four constructs, each containing two copies of EIII fused to flagellin (R3.2x format), elicited robust and long-lived neutralizing antibodies (geometric mean titers of 200 to 3,000), as measured with a 50% focus reduction neutralization test (FRNT50). In an immunogenicity study, rhesus macaques (n = 2) immunized subcutaneously with 10 μg or 90 μg of TDV three or four times, at 4- to 6-week intervals, developed neutralizing antibodies to four dengue virus (DENV) serotypes (mean post-dose 3 FRNT50 titers of 102 to 601). In an efficacy study, rhesus macaques (n = 4) were immunized intramuscularly with 16 μg or 48 μg of TDV or a placebo control three times, at 1-month intervals. The animals that received 48-μg doses of TDV developed neutralizing antibodies against the four serotypes (geometric mean titers of 49 to 258) and exhibited reduced viremia after DENV-2 challenge, with a group mean viremia duration of 1.25 days and 2 of 4 animals being completely protected, compared to the placebo-treated animals, which all developed viremia, with a mean duration of 4 days. In conclusion, flagellin-EIII fusion vaccines are immunogenic and partially protective in a nonhuman primate model.

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عنوان ژورنال:
  • Clinical and vaccine immunology : CVI

دوره 22 5  شماره 

صفحات  -

تاریخ انتشار 2015