| Literature DB >> 28794027 |
Qifeng Han1, Wilton B Williams1, Kevin O Saunders1, Kelly E Seaton1, Kevin J Wiehe1, Nathan Vandergrift1, Tarra A Von Holle1, Ashley M Trama1, Robert J Parks1, Kan Luo1, Thaddeus C Gurley1, Thomas B Kepler2, Dawn J Marshall1, David C Montefiori1, Laura L Sutherland1, Munir S Alam1, John F Whitesides1, Cindy M Bowman1, Sallie R Permar1, Barney S Graham3, John R Mascola3, Patrick C Seed4, Koen K A Van Rompay5, Georgia D Tomaras1, M Anthony Moody1, Barton F Haynes6.
Abstract
Dominant antibody responses in vaccinees who received the HIV-1 multiclade (A, B, and C) envelope (Env) DNA/recombinant adenovirus virus type 5 (rAd5) vaccine studied in HIV-1 Vaccine Trials Network (HVTN) efficacy trial 505 (HVTN 505) targeted Env gp41 and cross-reacted with microbial antigens. In this study, we asked if the DNA/rAd5 vaccine induced a similar antibody response in rhesus macaques (RMs), which are commonly used as an animal model for human HIV-1 infections and for testing candidate HIV-1 vaccines. We also asked if gp41 immunodominance could be avoided by immunization of neonatal RMs during the early stages of microbial colonization. We found that the DNA/rAd5 vaccine elicited a higher frequency of gp41-reactive memory B cells than gp120-memory B cells in adult and neonatal RMs. Analysis of the vaccine-induced Env-reactive B cell repertoire revealed that the majority of HIV-1 Env-reactive antibodies in both adult and neonatal RMs were targeted to gp41. Interestingly, a subset of gp41-reactive antibodies isolated from RMs cross-reacted with host antigens, including autologous intestinal microbiota. Thus, gp41-containing DNA/rAd5 vaccine induced dominant gp41-microbiota cross-reactive antibodies derived from blood memory B cells in RMs as observed in the HVTN 505 vaccine efficacy trial. These data demonstrated that RMs can be used to investigate gp41 immunodominance in candidate HIV-1 vaccines. Moreover, colonization of neonatal RMs occurred within the first week of life, and immunization of neonatal RMs during this time also induced a dominant gp41-reactive antibody response.IMPORTANCE Our results are critical to current work in the HIV-1 vaccine field evaluating the phenomenon of gp41 immunodominance induced by HIV-1 Env gp140 in RMs and humans. Our data demonstrate that RMs are an appropriate animal model to study this phenomenon and to determine the immunogenicity in new HIV-1 Env trimer vaccine designs. The demonstration of gp41 immunodominance in memory B cells of both adult and neonatal RMs indicated that early vaccination could not overcome gp41 dominant responses.Entities:
Keywords: HIV-1 envelope; HIV-1 vaccine; gp41; microbiome; rhesus macaques
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Year: 2017 PMID: 28794027 PMCID: PMC5640856 DOI: 10.1128/JVI.00923-17
Source DB: PubMed Journal: J Virol ISSN: 0022-538X Impact factor: 6.549