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Reproducing SIV?nef vaccine correlates of protection: trimeric gp41 antibody concentrated at mucosal front lines.


ABSTRACT: Vaccination with SIVmac239?nef provides robust protection against subsequent challenge with wild-type simian immunodeficiency virus (SIV), but safety issues have precluded designing an HIV-1 vaccine based on a live-attenuated virus concept. Safe immunogens and adjuvants that could reproduce identified immune correlates of SIVmac239?nef protection therefore offer an alternative path for development of an HIV vaccine. Here we describe SIV envelope trimeric gp41 (gp41t) immunogens based on a protective correlate of antibodies to gp41t concentrated on the path of virus entry by the neonatal Fc receptor (FcRn) in cervical vaginal epithelium. We developed a gp41t immunogen-monophosphoryl lipid A adjuvant liposomal nanoparticle for intramuscular (i.m.) immunization and a gp41t-Fc immunogen for intranasal immunization for pilot studies in mice, rabbits, and rhesus macaques. Repeated immunizations to mimic persistent antigen exposure in infection elicited gp41t antibodies in rhesus macaques that were detectable in FcRn+ cervical vaginal epithelium, thus recapitulating one key feature of SIVmac239?nef vaccinated and protected animals. Although this strategy did not reproduce the system of local production of antibody in SIVmac239?nef-vaccinated animals, passive immunization experiments supported the concept that sufficiently high levels of antibody can be concentrated by the FcRn at mucosal frontlines, thus setting the stage for assessing protection against vaginal challenge by gp41t immunization.

SUBMITTER: Voss JE 

PROVIDER: S-EPMC5069161 | biostudies-literature | 2016 Oct

REPOSITORIES: biostudies-literature

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Reproducing SIVΔnef vaccine correlates of protection: trimeric gp41 antibody concentrated at mucosal front lines.

Voss James E JE   Macauley Matthew S MS   Rogers Kenneth A KA   Villinger Francois F   Duan Lijie L   Shang Liang L   Fink Elizabeth A EA   Andrabi Raiees R   Colantonio Arnaud D AD   Robinson James E JE   Johnson R Paul RP   Burton Dennis R DR   Haase Ashley T AT  

AIDS (London, England) 20161001 16


Vaccination with SIVmac239Δnef provides robust protection against subsequent challenge with wild-type simian immunodeficiency virus (SIV), but safety issues have precluded designing an HIV-1 vaccine based on a live-attenuated virus concept. Safe immunogens and adjuvants that could reproduce identified immune correlates of SIVmac239Δnef protection therefore offer an alternative path for development of an HIV vaccine. Here we describe SIV envelope trimeric gp41 (gp41t) immunogens based on a protec  ...[more]

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