AI Article Synopsis

  • The study tested a prime/boost HIV vaccine strategy using 5 lipopeptides (HIV-Lipo-5) and a modified vaccinia virus (rMVA-HIV) in cynomolgus macaques.
  • Both vaccine components showed excellent safety, with HIV-Lipo-5 significantly raising anti-HIV antibody levels, while strong T-cell responses needed the combination with rMVA-HIV, particularly against the Gag antigen.
  • The results suggest that using HIV-Lipo-5 for initial priming followed by rMVA-HIV as a booster could be an effective strategy for preventing or treating HIV/AIDS.

Article Abstract

We evaluated the immunogenicity of a prime/boost vaccine strategy combining 5 lipopeptides (HIV-Lipo-5) and a recombinant modified vaccinia virus Ankara (rMVA-HIV) in cynomolgus macaques. Both of these vaccine components deliver HIV LAI Gag, Pol, and Nef antigens. Systemic and local safety was excellent in all groups. Immunization with HIV-Lipo-5 alone induced significant serum anti-HIV antibody titers which were not modified by rMVA-HIV immunization. However, induction of T-cell responses, as measured by IFNγ and IL-2 producing cells upon short-term stimulation with HIV peptide pools, required combined immunization with rMVA-HIV. Responses were preferentially observed against Gag antigen. Interestingly, HIV-Lipo-5 efficiently primed HIV induced T-cell responses upon the injection of rMVA-HIV, which may help to reduce the required number of vector injections. Our results provide a rationale for the use of a strategy involving HIV-Lipo-5 priming followed by rMVA-HIV booster immunization as a prophylactic or therapeutic vaccine approach against HIV infection and AIDS.

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Source
http://dx.doi.org/10.1016/j.vaccine.2015.03.032DOI Listing

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