PLoS ONE (Jan 2018)

Mucosal antibody responses to vaccines targeting SIV protease cleavage sites or full-length Gag and Env proteins in Mauritian cynomolgus macaques.

  • Hongzhao Li,
  • Yan Hai,
  • So-Yon Lim,
  • Nikki Toledo,
  • Jose Crecente-Campo,
  • Dane Schalk,
  • Lin Li,
  • Robert W Omange,
  • Tamara G Dacoba,
  • Lewis R Liu,
  • Mohammad Abul Kashem,
  • Yanmin Wan,
  • Binhua Liang,
  • Qingsheng Li,
  • Eva Rakasz,
  • Nancy Schultz-Darken,
  • Maria J Alonso,
  • Francis A Plummer,
  • James B Whitney,
  • Ma Luo

DOI
https://doi.org/10.1371/journal.pone.0202997
Journal volume & issue
Vol. 13, no. 8
p. e0202997

Abstract

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HIV mutates rapidly and infects CD4+ T cells, especially when they are activated. A vaccine targeting conserved, essential viral elements while limiting CD4+ T cell activation could be effective. Learning from natural immunity observed in a group of highly HIV-1 exposed seronegative Kenyan female sex workers, we are testing a novel candidate HIV vaccine targeting the 12 viral protease cleavage sites (PCSs) (the PCS vaccine), in comparison with a vaccine targeting full-length Gag and Env (the Gag/Env vaccine) in a Mauritian cynomolgus macaque/SIV model. In this study we evaluated these vaccines for induction of mucosal antibodies to SIV immunogens at the female genital tract. Bio-Plex and Western blot analyses of cervicovaginal lavage samples showed that both the PCS and Gag/Env vaccines can elicit mucosal IgG antibody responses to SIV immunogens. Significantly higher increase of anti-PCS antibodies was induced by the PCS vaccine than by the Gag/Env vaccine (p<0.0001). The effect of the mucosal antibody responses in protection from repeated low dose pathogenic SIVmac251 challenges is being evaluated.