Vaccine-Induced Env V1-V2 IgG3 Correlates with Lower HIV-1 Infection Risk and Declines Soon After Vaccination

Nicole L. Yates; Hua-Xin Liao; Youyi Fong; Allan C. deCamp; Nathan Vandergrift; William T. Williams; S. Munir Alam; Guido Ferrari; Zhi-Yong Yang; Kelly E. Seaton; Phillip W. Berman; Michael D. Alpert; David T. Evans; Robert J. O’Connell; Donald P. Francis; Faruk Sinangil; Carter Lee; Sorachai Nitayaphan; Supachai Rerks‐Ngarm; Jaranit Kaewkungwal; Punnee Pitisuttithum; James Tartaglia; Abraham Pinter; Susan Zolla‐Pazner; Peter B. Gilbert; Gary J. Nabel; Nelson L. Michael; Jérôme H. Kim; David C. Montefiori; Barton F. Haynes; Georgia D. Tomaras

doi:10.1126/scitranslmed.3007730

Vaccine-Induced Env V1-V2 IgG3 Correlates with Lower HIV-1 Infection Risk and Declines Soon After Vaccination

Nicole L. Yates(Duke University), Hua-Xin Liao(Duke University), Youyi Fong(Fred Hutch Cancer Center), Allan C. deCamp(Fred Hutch Cancer Center), Nathan Vandergrift(Duke University), William T. Williams(Duke University), S. Munir Alam(Duke University), Guido Ferrari(Duke University), Zhi-Yong Yang(National Institutes of Health), Kelly E. Seaton(Duke University), Phillip W. Berman(University of California, Santa Cruz), Michael D. Alpert(Harvard University), David T. Evans(Harvard University), Robert J. O’Connell(Armed Forces Research Institute of Medical Science), Donald P. Francis(Global Solutions for Infectious Diseases), Faruk Sinangil(Global Solutions for Infectious Diseases), Carter Lee(Global Solutions for Infectious Diseases), Sorachai Nitayaphan(Armed Forces Research Institute of Medical Science), Supachai Rerks‐Ngarm(Ministry of Public Health), Jaranit Kaewkungwal(Mahidol University), Punnee Pitisuttithum(Mahidol University), James Tartaglia(Sanofi (United States)), Abraham Pinter(Rutgers, The State University of New Jersey), Susan Zolla‐Pazner(Veterans Health Administration), Peter B. Gilbert(Fred Hutch Cancer Center), Gary J. Nabel(National Institutes of Health), Nelson L. Michael(Walter Reed Army Institute of Research), Jérôme H. Kim(Walter Reed Army Institute of Research), David C. Montefiori(Duke University), Barton F. Haynes(Duke University), Georgia D. Tomaras(Duke University)

Science Translational Medicine

March 19, 2014

10.1126/scitranslmed.3007730

Cited by 453

Abstract

HIV-1-specific immunoglobulin G (IgG) subclass antibodies bind to distinct cellular Fc receptors. Antibodies of the same epitope specificity but of a different subclass therefore can have different antibody effector functions. The study of IgG subclass profiles between different vaccine regimens used in clinical trials with divergent efficacy outcomes can provide information on the quality of the vaccine-induced B cell response. We show that HIV-1-specific IgG3 distinguished two HIV-1 vaccine efficacy studies (RV144 and VAX003 clinical trials) and correlated with decreased risk of HIV-1 infection in a blinded follow-up case-control study with the RV144 vaccine. HIV-1-specific IgG3 responses were not long-lived, which was consistent with the waning efficacy of the RV144 vaccine. These data suggest that specific vaccine-induced HIV-1 IgG3 should be tested in future studies of immune correlates in HIV-1 vaccine efficacy trials.

Related Papers

No related papers found

Powered by citation graph analysis