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Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost

In the RV144 trial, to date the only HIV-1 vaccine efficacy trial demonstrating a modestly reduced risk of HIV-1 acquisition, antibody responses toward the HIV Envelope protein (Env) variable (V) 2 and V3 regions were shown to be correlated with a reduced risk of infection. These potentially protect...

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Autores principales: Joachim, Agricola, Ahmed, Mohamed I. M., Pollakis, Georgios, Rogers, Lisa, Hoffmann, Verena S., Munseri, Patricia, Aboud, Said, Lyamuya, Eligius F., Bakari, Muhammad, Robb, Merlin L., Wahren, Britta, Sandstrom, Eric, Nilsson, Charlotta, Biberfeld, Gunnel, Geldmacher, Christof, Held, Kathrin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7198863/
https://www.ncbi.nlm.nih.gov/pubmed/32411138
http://dx.doi.org/10.3389/fimmu.2020.00719
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author Joachim, Agricola
Ahmed, Mohamed I. M.
Pollakis, Georgios
Rogers, Lisa
Hoffmann, Verena S.
Munseri, Patricia
Aboud, Said
Lyamuya, Eligius F.
Bakari, Muhammad
Robb, Merlin L.
Wahren, Britta
Sandstrom, Eric
Nilsson, Charlotta
Biberfeld, Gunnel
Geldmacher, Christof
Held, Kathrin
author_facet Joachim, Agricola
Ahmed, Mohamed I. M.
Pollakis, Georgios
Rogers, Lisa
Hoffmann, Verena S.
Munseri, Patricia
Aboud, Said
Lyamuya, Eligius F.
Bakari, Muhammad
Robb, Merlin L.
Wahren, Britta
Sandstrom, Eric
Nilsson, Charlotta
Biberfeld, Gunnel
Geldmacher, Christof
Held, Kathrin
author_sort Joachim, Agricola
collection PubMed
description In the RV144 trial, to date the only HIV-1 vaccine efficacy trial demonstrating a modestly reduced risk of HIV-1 acquisition, antibody responses toward the HIV Envelope protein (Env) variable (V) 2 and V3 regions were shown to be correlated with a reduced risk of infection. These potentially protective antibody responses, in parallel with the vaccine efficacy, however, waned quickly. Dissecting vaccine-induced IgG recognition of antigenic regions and their variants within the HIV-1 Env from different vaccine trials will aid in designing future HIV-1 immunogens and vaccination schedules. We, therefore, analyzed the IgG response toward linear HIV-1 Env epitopes elicited by a multi-clade, multigene HIVIS-DNA priming, and heterologous recombinant modified vaccinia virus Ankara (MVA-CMDR) boosting regimen (HIVIS03) and assessed whether a late MVA-CMDR boost 3 years after completion of the initial vaccination schedule (HIVIS06) restored antibody responses toward these epitopes. Here we report that vaccination schedule in the HIVIS03 trial elicited IgG responses against linear epitopes within the V2 and V3 tip as well as against the gp41 immunodominant region in a high proportion of vaccinees. Antibodies against the V2 and gp41 Env regions were restricted to variants with close homology to the MVA-CMDR immunogen sequence, while V3 responses were more cross-reactive. Boosting with a late third MVA-CMDR after 3 years effectively restored waned IgG responses to linear Env epitopes and induced targeting of identical antigenic regions and variants comparable to the previous combined HIVIS-DNA/MVA-CMDR regimen. Our findings support the notion that anti-HIV-1 Env responses, associated with a reduced risk of infection in RV144, could be maintained by regular boosting with a single dose of MVA-CMDR.
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spelling pubmed-71988632020-05-14 Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost Joachim, Agricola Ahmed, Mohamed I. M. Pollakis, Georgios Rogers, Lisa Hoffmann, Verena S. Munseri, Patricia Aboud, Said Lyamuya, Eligius F. Bakari, Muhammad Robb, Merlin L. Wahren, Britta Sandstrom, Eric Nilsson, Charlotta Biberfeld, Gunnel Geldmacher, Christof Held, Kathrin Front Immunol Immunology In the RV144 trial, to date the only HIV-1 vaccine efficacy trial demonstrating a modestly reduced risk of HIV-1 acquisition, antibody responses toward the HIV Envelope protein (Env) variable (V) 2 and V3 regions were shown to be correlated with a reduced risk of infection. These potentially protective antibody responses, in parallel with the vaccine efficacy, however, waned quickly. Dissecting vaccine-induced IgG recognition of antigenic regions and their variants within the HIV-1 Env from different vaccine trials will aid in designing future HIV-1 immunogens and vaccination schedules. We, therefore, analyzed the IgG response toward linear HIV-1 Env epitopes elicited by a multi-clade, multigene HIVIS-DNA priming, and heterologous recombinant modified vaccinia virus Ankara (MVA-CMDR) boosting regimen (HIVIS03) and assessed whether a late MVA-CMDR boost 3 years after completion of the initial vaccination schedule (HIVIS06) restored antibody responses toward these epitopes. Here we report that vaccination schedule in the HIVIS03 trial elicited IgG responses against linear epitopes within the V2 and V3 tip as well as against the gp41 immunodominant region in a high proportion of vaccinees. Antibodies against the V2 and gp41 Env regions were restricted to variants with close homology to the MVA-CMDR immunogen sequence, while V3 responses were more cross-reactive. Boosting with a late third MVA-CMDR after 3 years effectively restored waned IgG responses to linear Env epitopes and induced targeting of identical antigenic regions and variants comparable to the previous combined HIVIS-DNA/MVA-CMDR regimen. Our findings support the notion that anti-HIV-1 Env responses, associated with a reduced risk of infection in RV144, could be maintained by regular boosting with a single dose of MVA-CMDR. Frontiers Media S.A. 2020-04-28 /pmc/articles/PMC7198863/ /pubmed/32411138 http://dx.doi.org/10.3389/fimmu.2020.00719 Text en Copyright © 2020 Joachim, Ahmed, Pollakis, Rogers, Hoffmann, Munseri, Aboud, Lyamuya, Bakari, Robb, Wahren, Sandstrom, Nilsson, Biberfeld, Geldmacher and Held. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Joachim, Agricola
Ahmed, Mohamed I. M.
Pollakis, Georgios
Rogers, Lisa
Hoffmann, Verena S.
Munseri, Patricia
Aboud, Said
Lyamuya, Eligius F.
Bakari, Muhammad
Robb, Merlin L.
Wahren, Britta
Sandstrom, Eric
Nilsson, Charlotta
Biberfeld, Gunnel
Geldmacher, Christof
Held, Kathrin
Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title_full Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title_fullStr Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title_full_unstemmed Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title_short Induction of Identical IgG HIV-1 Envelope Epitope Recognition Patterns After Initial HIVIS-DNA/MVA-CMDR Immunization and a Late MVA-CMDR Boost
title_sort induction of identical igg hiv-1 envelope epitope recognition patterns after initial hivis-dna/mva-cmdr immunization and a late mva-cmdr boost
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7198863/
https://www.ncbi.nlm.nih.gov/pubmed/32411138
http://dx.doi.org/10.3389/fimmu.2020.00719
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