Recombinant MVA-prime elicits neutralizing antibody responses by inducing antigen-specific B cells in the germinal center

Author:

Eslamizar Leila,Petrovas ConstantinosORCID,Leggat David J.ORCID,Furr Kathryn,Lifton Michelle L.ORCID,Levine Gail,Ma Steven,Fletez-Brant ChristopherORCID,Hoyland Wesley,Prabhakaran Madhu,Narpala Sandeep,Boswell Kristin,Yamamoto TakuyaORCID,Liao Hua-Xin,Pickup David,Ramsburg Elizabeth,Sutherland Laura,McDermott AdrianORCID,Roederer Mario,Montefiori David,Koup Richard A.,Haynes Barton F.,Letvin Norman L.,Santra SampaORCID

Abstract

AbstractThe RV144 HIV-1 vaccine trial has been the only clinical trial to date that has shown any degree of efficacy and associated with the presence of vaccine-elicited HIV-1 envelope-specific binding antibody and CD4+ T-cell responses. This trial also showed that a vector-prime protein boost combined vaccine strategy was better than when used alone. Here we have studied three different priming vectors—plasmid DNA, recombinant MVA, and recombinant VSV, all encoding clade C transmitted/founder Env 1086 C gp140, for priming three groups of six non-human primates each, followed by a protein boost with adjuvanted 1086 C gp120 protein. Our data showed that MVA-priming favors the development of higher antibody binding titers and neutralizing activity compared with other vectors. Analyses of the draining lymph nodes revealed that MVA-prime induced increased germinal center reactivity characterized by higher frequencies of germinal center (PNAhi) B cells, higher frequencies of antigen-specific B-cell responses as well as an increased frequency of the highly differentiated (ICOShiCD150lo) Tfh-cell subset.

Funder

U.S. Department of Health & Human Services | NIH | National Institute of Allergy and Infectious Diseases

Bill and Melinda Gates Foundation

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

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