Article
作者: Stanley, Kelly A ; Tomaka, Frank ; Borducchi, Erica N ; Pegu, Poonam ; Kinney, Amy ; Kirilova, Marinela ; Nichols, James ; Dominguez, David J ; Pau, Maria G ; Mei, Chun Su ; Hamel, Robyn ; Kleinjan, Jane A ; Licona, J Humberto ; Engelson, Brian ; Walsh, Stephen R ; Ganley, Sarah ; Barouch, Dan H ; Gothing, Jon A ; Ghantous, Fadi ; Liakos, Alexis ; Stephenson, Kathryn E ; Cohen, Yehuda Z ; Roten, Raphaele ; Brandariz, Kara ; Hodin, Caroline ; Johnson, Jennifer A ; Peter, Lauren ; Buleza, Karen ; Zinchuk, Kevin ; LaPorte, Annalena ; Baden, Lindsey R ; Nkolola, Joseph ; Hendriks, Jenny ; Filter, Rachel D ; Robles, Alexander ; Weijtens, Mo ; Iampietro, Mark J ; Nijs, Steven ; Yuan, Olive ; Garrity, Jetta ; Rist, Michael ; Shields, Jennifer ; Lavine, Christy L ; Eller, Michael A ; Callewaert, Katleen ; Schuitemaker, Hanneke ; Alter, Galit ; Dolin, Raphael ; Trinh, Hung V ; Robb, Merlin L ; Ake, Julie A ; Korber, Bette T ; Seaman, Michael S ; Abbink, Peter ; Sarnecki, Michal ; Cheung, Ann ; Patel, Alka ; Rao, Mangala ; Scheppler, Lorenz ; Michael, Nelson L ; Wajima, Makoto ; McNally, Anna G ; Euler, Zelda ; Zingg, Marshall ; Moss, Bernard ; Bayne, Madeline ; Huskens, Gitta ; Earl, Patricia L ; Dilan, Rebecca ; Fredette, Nicholas ; Stephens, Faye ; Yanosick, Katherine E ; Muller, Heidi ; Jennings, Julia ; Gadre, Soniya
BackgroundMosaic immunogens are bioinformatically engineered human immunodeficiency virus type 1 (HIV-1) sequences designed to elicit clade-independent coverage against globally circulating HIV-1 strains.MethodsThis phase 1, double-blinded, randomized, placebo-controlled trial enrolled healthy HIV-uninfected adults who received 2 doses of a modified vaccinia Ankara (MVA)-vectored HIV-1 bivalent mosaic immunogen vaccine or placebo on days 0 and 84. Two groups were enrolled: those who were HIV-1 vaccine naive (n = 15) and those who had received an HIV-1 vaccine (Ad26.ENVA.01) 4-6 years earlier (n = 10). We performed prespecified blinded cellular and humoral immunogenicity analyses at days 0, 14, 28, 84, 98, 112, 168, 270, and 365.ResultsAll 50 planned vaccinations were administered. Vaccination was safe and generally well tolerated. No vaccine-related serious adverse events occurred. Both cellular and humoral cross-clade immune responses were elicited after 1 or 2 vaccinations in all participants in the HIV-1 vaccine-naive group. Env-specific responses were induced after a single immunization in nearly all subjects who had previously received the prototype Ad26.ENVA.01 vaccine.ConclusionsNo safety concerns were identified, and multiclade HIV-1-specific immune responses were elicited.Clinical Trials RegistrationNCT02218125.