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  • Humoral immunity induced by mucosal and/or systemic SIV-specific vaccine platforms suggests novel combinatorial approaches for enhancing responses.

Humoral immunity induced by mucosal and/or systemic SIV-specific vaccine platforms suggests novel combinatorial approaches for enhancing responses.

Clinical immunology (Orlando, Fla.) (2014-06-08)
Diego A Vargas-Inchaustegui, Iskra Tuero, Venkatramanan Mohanram, Thomas Musich, Poonam Pegu, Antonio Valentin, Yongjun Sui, Margherita Rosati, Jenifer Bear, David J Venzon, Viraj Kulkarni, Candido Alicea, Guy R Pilkington, Namal P M Liyanage, Thorsten Demberg, Shari N Gordon, Yichuan Wang, Alison E Hogg, Blake Frey, L Jean Patterson, Janet DiPasquale, David C Montefiori, Niranjan Y Sardesai, Steven G Reed, Jay A Berzofsky, Genoveffa Franchini, Barbara K Felber, George N Pavlakis, Marjorie Robert-Guroff
ABSTRACT

Combinatorial HIV/SIV vaccine approaches targeting multiple arms of the immune system might improve protective efficacy. We compared SIV-specific humoral immunity induced in rhesus macaques by five vaccine regimens. Systemic regimens included ALVAC-SIVenv priming and Env boosting (ALVAC/Env); DNA immunization; and DNA plus Env co-immunization (DNA&Env). RepAd/Env combined mucosal replication-competent Ad-env priming with systemic Env boosting. A Peptide/Env regimen, given solely intrarectally, included HIV/SIV peptides followed by MVA-env and Env boosts. Serum antibodies mediating neutralizing, phagocytic and ADCC activities were induced by ALVAC/Env, RepAd/Env and DNA&Env vaccines. Memory B cells and plasma cells were maintained in the bone marrow. RepAd/Env vaccination induced early SIV-specific IgA in rectal secretions before Env boosting, although mucosal IgA and IgG responses were readily detected at necropsy in ALVAC/Env, RepAd/Env, DNA&Env and DNA vaccinated animals. Our results suggest that combined RepAd priming with ALVAC/Env or DNA&Env regimen boosting might induce potent, functional, long-lasting systemic and mucosal SIV-specific antibodies.