Piyathida Sroysuwan, Natthapol Kosashunhanan, Sebastian Molnar, Jerome H. Kim, Alexandra Schuetz, Taweewat Supindham, Elizabeth Heger, Sandhya Vasan, Phiromrat Rakyat, Suwat Chariyalertsak, Nittaya Phanuphak, Siriluck Teerachia, Suchada Chinaworapong, Nongluck Sangnoi, Oranitcha Kaewthip, Sorachai Nitayaphan, Surat Jongrakthaitae, Pornchanok Panjapornsuk, Michael A. Eller, Puttachard Saengtawan, Weerawan Chuenarom, Nuntisa Chotirosniramit, Pornsuk V. Grandin, Sirinan Madnote, Benjaluck Phonrat, Rungsun Rerknimitr, Narongrid Sirisopana, Lindsay Wieczorek, Siriwat Akapirat, Chirapa Eamsila, Faruk Sinangil, Kirsten Smith, James Tartaglia, Poonam Pegu, Dohoon Kim, Carter Lee, Peter Dawson, Saowanit Getchalarat, Robert J. O'Connell, Nicos Karasavvas, Jiraporn Puangkaew, Patcharaphan Sugandhavesa, Nitiya Chomchey, Punnee Pitisuttithum, Jean-Louis Excler, Boonlure Pruenglampoo, Yingjun Zhou, Yupa Sabmee, Jittima Dhitavat, Merlin L. Robb, Jesse Schoen, Victoria R. Polonis, Nelson L. Michael, Boot Kaewboon, Nipat Teeratakulpisarn, Bessara Nuntapinit, Wanlaya Labwech, Eugene Kroon, Viseth Ngauy, Prapaporn Savaraj, Jaranit Kaewkungwal, Pawinee Jarujareet, Nampueng Churikanont, Surawach Rittiroongrad, Somsak Chantakulkij, Anant Phramtong, Rapee Trichavaroj, Carlos A. DiazGranados, Silvia Ratto-Kim, Sanjay Phogat, Mark de Souza, Arom Pitisuthitham, and Nipattra Tragonlugsana
BACKGROUND: The RV144 phase 3 vaccine trial in Thailand demonstrated that ALVAC-HIV (vCP1521) and AIDSVAX® B/E administration over six months resulted in a 31% efficacy in preventing HIV acquisition. In this trial, we assessed the immunologic impact of an additional vaccine boost to the RV144 regimen at varying intervals between the priming vaccine series and the boost. METHODS: RV306 is a double-blind, placebo-controlled, randomized clinical trial conducted in three clinical sites in Thailand. HIV-uninfected volunteers aged 20–40 randomly received the primary RV144 vaccine series at months 0, 1, 3, and 6, with no additional boost (Group I), additional AIDSVAX® B/E and ALVAC-HIV (vcp1521) at month 12 (Group II), AIDSVAX® B/E alone at month 12 (Group III), AIDSVAX® B/E and ALVAC-HIV at month 15 or 18 (Groups IVa or IVb), or placebo and were followed for 24 months. A randomization schedule was centrally generated with fixed sized strata for RIHES Chiang Mai (n=60) and combined Bangkok clinics (n=300). Primary outcomes were to assess the safety and tolerability of these vaccination regimens and characterize and compare cellular and humoral immune responses between the RV144 series alone and late boosts at different timepoints. Safety and tolerability outcomes were assessed by evaluating local and systemic reactogenicity and adverse events in all participants. Primary immunogenicity outcomes were evaluated by comparing peak humoral responses (HIV-specific IgG and IgA ELISA) and cellular responses (HIV-specific intracellular cytokine staining and polyfunctionality) two weeks post final vaccination among per-protocol participants who completed all vaccinations. This trial is registered at (ClinicalTrials.gov (NCT01931358); clinical follow up is now complete. FINDINGS: Between 28 October 2013 and 29 April 2014, 367 participants were enrolled, of whom 27 were assigned active vaccination in Group I, 102 in Group II, 101 in Group III, 52 in Group IVa, 51 in Group IVb, and 34 combined placebo across all groups. Late boosting did not induce vaccine-related serious adverse events. There were no significant differences in the occurrence or severity of local or systemic reactogenicity across active groups. Groups with late boosts (Groups II, III, IVa, and IVb) had increased peak plasma IgG binding antibody levels against gp70 V1V2 relative to Group I vaccine recipients with no late boost (gp70V1V2 92TH023 adjusted p < 0·02 for each; gp70V1V2 Case A2 adjusted p month 15 (Group IVa) > month 12 (Groups II+III) > no late boost (Group I). Groups with late boosts had increased both functionality and polyfunctionality scores relative to vaccine recipients with no late boost (all adjusted p < 0·05, except for polyfunctionality score in Group I vs in Group IVb p < 0·01). INTERPRETATION: Taken together, these results suggest that additional boosting of the RV144 regimen with longer intervals between the primary vaccination series and late boost improved immune responses and may improve the efficacy of preventing HIV acquisition. FUNDING: US National Institute of Allergy and Infectious Diseases (NIAID) and U.S. Department of the Army.