Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial

BACKGROUND: Intradermal priming with HIV-1 DNA plasmids followed by HIV-1MVA boosting induces strong and broad cellular and humoral immune responses. In our previous HIVIS-03 trial, we used 5 injections with 2 pools of HIV-DNA at separate sites for each priming immunization. The present study explor...

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Autores principales: Munseri, Patricia. J., Kroidl, Arne, Nilsson, Charlotta, Joachim, Agricola, Geldmacher, Christof, Mann, Philipp, Moshiro, Candida, Aboud, Said, Lyamuya, Eligius, Maboko, Leonard, Missanga, Marco, Kaluwa, Bahati, Mfinanga, Sayoki, Podola, Lilly, Bauer, Asli, Godoy-Ramirez, Karina, Marovich, Mary, Moss, Bernard, Hoelscher, Michael, Gotch, Frances, Stöhr, Wolfgang, Stout, Richard, McCormack, Sheena, Wahren, Britta, Mhalu, Fred, Robb, Merlin L., Biberfeld, Gunnel, Sandström, Eric, Bakari, Muhammad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4398367/
https://www.ncbi.nlm.nih.gov/pubmed/25875843
http://dx.doi.org/10.1371/journal.pone.0119629
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author Munseri, Patricia. J.
Kroidl, Arne
Nilsson, Charlotta
Joachim, Agricola
Geldmacher, Christof
Mann, Philipp
Moshiro, Candida
Aboud, Said
Lyamuya, Eligius
Maboko, Leonard
Missanga, Marco
Kaluwa, Bahati
Mfinanga, Sayoki
Podola, Lilly
Bauer, Asli
Godoy-Ramirez, Karina
Marovich, Mary
Moss, Bernard
Hoelscher, Michael
Gotch, Frances
Stöhr, Wolfgang
Stout, Richard
McCormack, Sheena
Wahren, Britta
Mhalu, Fred
Robb, Merlin L.
Biberfeld, Gunnel
Sandström, Eric
Bakari, Muhammad
author_facet Munseri, Patricia. J.
Kroidl, Arne
Nilsson, Charlotta
Joachim, Agricola
Geldmacher, Christof
Mann, Philipp
Moshiro, Candida
Aboud, Said
Lyamuya, Eligius
Maboko, Leonard
Missanga, Marco
Kaluwa, Bahati
Mfinanga, Sayoki
Podola, Lilly
Bauer, Asli
Godoy-Ramirez, Karina
Marovich, Mary
Moss, Bernard
Hoelscher, Michael
Gotch, Frances
Stöhr, Wolfgang
Stout, Richard
McCormack, Sheena
Wahren, Britta
Mhalu, Fred
Robb, Merlin L.
Biberfeld, Gunnel
Sandström, Eric
Bakari, Muhammad
author_sort Munseri, Patricia. J.
collection PubMed
description BACKGROUND: Intradermal priming with HIV-1 DNA plasmids followed by HIV-1MVA boosting induces strong and broad cellular and humoral immune responses. In our previous HIVIS-03 trial, we used 5 injections with 2 pools of HIV-DNA at separate sites for each priming immunization. The present study explores whether HIV-DNA priming can be simplified by reducing the number of DNA injections and administration of combined versus separated plasmid pools. METHODS: In this phase IIa, randomized trial, priming was performed using 5 injections of HIV-DNA, 1000 μg total dose, (3 Env and 2 Gag encoding plasmids) compared to two “simplified” regimens of 2 injections of HIV-DNA, 600 μg total dose, of Env- and Gag-encoding plasmid pools with each pool either administered separately or combined. HIV-DNA immunizations were given intradermally at weeks 0, 4, and 12. Boosting was performed intramuscularly with 10(8) pfu HIV-MVA at weeks 30 and 46. RESULTS: 129 healthy Tanzanian participants were enrolled. There were no differences in adverse events between the groups. The proportion of IFN-γ ELISpot responders to Gag and/or Env peptides after the second HIV-MVA boost did not differ significantly between the groups primed with 2 injections of combined HIV-DNA pools, 2 injections with separated pools, and 5 injections with separated pools (90%, 97% and 97%). There were no significant differences in the magnitude of Gag and/or Env IFN-γ ELISpot responses, in CD4+ and CD8+ T cell responses measured as IFN-γ/IL-2 production by intracellular cytokine staining (ICS) or in response rates and median titers for binding antibodies to Env gp160 between study groups. CONCLUSIONS: A simplified intradermal vaccination regimen with 2 injections of a total of 600 μg with combined HIV-DNA plasmids primed cellular responses as efficiently as the standard regimen of 5 injections of a total of 1000 μg with separated plasmid pools after boosting twice with HIV-MVA. TRIAL REGISTRATION: World Health Organization International Clinical Trials Registry Platform PACTR2010050002122368
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spelling pubmed-43983672015-04-21 Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial Munseri, Patricia. J. Kroidl, Arne Nilsson, Charlotta Joachim, Agricola Geldmacher, Christof Mann, Philipp Moshiro, Candida Aboud, Said Lyamuya, Eligius Maboko, Leonard Missanga, Marco Kaluwa, Bahati Mfinanga, Sayoki Podola, Lilly Bauer, Asli Godoy-Ramirez, Karina Marovich, Mary Moss, Bernard Hoelscher, Michael Gotch, Frances Stöhr, Wolfgang Stout, Richard McCormack, Sheena Wahren, Britta Mhalu, Fred Robb, Merlin L. Biberfeld, Gunnel Sandström, Eric Bakari, Muhammad PLoS One Research Article BACKGROUND: Intradermal priming with HIV-1 DNA plasmids followed by HIV-1MVA boosting induces strong and broad cellular and humoral immune responses. In our previous HIVIS-03 trial, we used 5 injections with 2 pools of HIV-DNA at separate sites for each priming immunization. The present study explores whether HIV-DNA priming can be simplified by reducing the number of DNA injections and administration of combined versus separated plasmid pools. METHODS: In this phase IIa, randomized trial, priming was performed using 5 injections of HIV-DNA, 1000 μg total dose, (3 Env and 2 Gag encoding plasmids) compared to two “simplified” regimens of 2 injections of HIV-DNA, 600 μg total dose, of Env- and Gag-encoding plasmid pools with each pool either administered separately or combined. HIV-DNA immunizations were given intradermally at weeks 0, 4, and 12. Boosting was performed intramuscularly with 10(8) pfu HIV-MVA at weeks 30 and 46. RESULTS: 129 healthy Tanzanian participants were enrolled. There were no differences in adverse events between the groups. The proportion of IFN-γ ELISpot responders to Gag and/or Env peptides after the second HIV-MVA boost did not differ significantly between the groups primed with 2 injections of combined HIV-DNA pools, 2 injections with separated pools, and 5 injections with separated pools (90%, 97% and 97%). There were no significant differences in the magnitude of Gag and/or Env IFN-γ ELISpot responses, in CD4+ and CD8+ T cell responses measured as IFN-γ/IL-2 production by intracellular cytokine staining (ICS) or in response rates and median titers for binding antibodies to Env gp160 between study groups. CONCLUSIONS: A simplified intradermal vaccination regimen with 2 injections of a total of 600 μg with combined HIV-DNA plasmids primed cellular responses as efficiently as the standard regimen of 5 injections of a total of 1000 μg with separated plasmid pools after boosting twice with HIV-MVA. TRIAL REGISTRATION: World Health Organization International Clinical Trials Registry Platform PACTR2010050002122368 Public Library of Science 2015-04-15 /pmc/articles/PMC4398367/ /pubmed/25875843 http://dx.doi.org/10.1371/journal.pone.0119629 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Munseri, Patricia. J.
Kroidl, Arne
Nilsson, Charlotta
Joachim, Agricola
Geldmacher, Christof
Mann, Philipp
Moshiro, Candida
Aboud, Said
Lyamuya, Eligius
Maboko, Leonard
Missanga, Marco
Kaluwa, Bahati
Mfinanga, Sayoki
Podola, Lilly
Bauer, Asli
Godoy-Ramirez, Karina
Marovich, Mary
Moss, Bernard
Hoelscher, Michael
Gotch, Frances
Stöhr, Wolfgang
Stout, Richard
McCormack, Sheena
Wahren, Britta
Mhalu, Fred
Robb, Merlin L.
Biberfeld, Gunnel
Sandström, Eric
Bakari, Muhammad
Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title_full Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title_fullStr Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title_full_unstemmed Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title_short Priming with a Simplified Intradermal HIV-1 DNA Vaccine Regimen followed by Boosting with Recombinant HIV-1 MVA Vaccine Is Safe and Immunogenic: A Phase IIa Randomized Clinical Trial
title_sort priming with a simplified intradermal hiv-1 dna vaccine regimen followed by boosting with recombinant hiv-1 mva vaccine is safe and immunogenic: a phase iia randomized clinical trial
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4398367/
https://www.ncbi.nlm.nih.gov/pubmed/25875843
http://dx.doi.org/10.1371/journal.pone.0119629
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