Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial

BACKGROUND: A vaccine against HIV is widely considered the most effective and sustainable way of reducing new infections. We evaluated the safety and impact of boosting with subtype C CN54rgp140 envelope protein adjuvanted in glucopyranosyl lipid adjuvant (GLA-AF) in Tanzanian volunteers previously...

Descripción completa

Detalles Bibliográficos
Autores principales: Joachim, Agricola, Bauer, Asli, Joseph, Sarah, Geldmacher, Christof, Munseri, Patricia J., Aboud, Said, Missanga, Marco, Mann, Philipp, Wahren, Britta, Ferrari, Guido, Polonis, Victoria R., Robb, Merlin L., Weber, Jonathan, Tatoud, Roger, Maboko, Leonard, Hoelscher, Michael, Lyamuya, Eligius F., Biberfeld, Gunnel, Sandström, Eric, Kroidl, Arne, Bakari, Muhammad, Nilsson, Charlotta, McCormack, Sheena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4871571/
https://www.ncbi.nlm.nih.gov/pubmed/27192151
http://dx.doi.org/10.1371/journal.pone.0155702
_version_ 1782432621447348224
author Joachim, Agricola
Bauer, Asli
Joseph, Sarah
Geldmacher, Christof
Munseri, Patricia J.
Aboud, Said
Missanga, Marco
Mann, Philipp
Wahren, Britta
Ferrari, Guido
Polonis, Victoria R.
Robb, Merlin L.
Weber, Jonathan
Tatoud, Roger
Maboko, Leonard
Hoelscher, Michael
Lyamuya, Eligius F.
Biberfeld, Gunnel
Sandström, Eric
Kroidl, Arne
Bakari, Muhammad
Nilsson, Charlotta
McCormack, Sheena
author_facet Joachim, Agricola
Bauer, Asli
Joseph, Sarah
Geldmacher, Christof
Munseri, Patricia J.
Aboud, Said
Missanga, Marco
Mann, Philipp
Wahren, Britta
Ferrari, Guido
Polonis, Victoria R.
Robb, Merlin L.
Weber, Jonathan
Tatoud, Roger
Maboko, Leonard
Hoelscher, Michael
Lyamuya, Eligius F.
Biberfeld, Gunnel
Sandström, Eric
Kroidl, Arne
Bakari, Muhammad
Nilsson, Charlotta
McCormack, Sheena
author_sort Joachim, Agricola
collection PubMed
description BACKGROUND: A vaccine against HIV is widely considered the most effective and sustainable way of reducing new infections. We evaluated the safety and impact of boosting with subtype C CN54rgp140 envelope protein adjuvanted in glucopyranosyl lipid adjuvant (GLA-AF) in Tanzanian volunteers previously given three immunizations with HIV-DNA followed by two immunizations with recombinant modified vaccinia virus Ankara (HIV-MVA). METHODS: Forty volunteers (35 vaccinees and five placebo recipients) were given two CN54rgp140/GLA-AF immunizations 30–71 weeks after the last HIV-MVA vaccination. These immunizations were delivered intramuscularly four weeks apart. RESULTS: The vaccine was safe and well tolerated except for one episode of asymptomatic hypoglycaemia that was classified as severe adverse event. Two weeks after the second HIV-MVA vaccination 34 (97%) of the 35 previously vaccinated developed Env-specific binding antibodies, and 79% and 84% displayed IFN-γ ELISpot responses to Gag and Env, respectively. Binding antibodies to subtype C Env (included in HIV-DNA and protein boost), subtype B Env (included only in HIV-DNA) and CRF01_AE Env (included only in HIV-MVA) were significantly boosted by the CN54rgp140/GLA-AF immunizations. Functional antibodies detected using an infectious molecular clone virus/peripheral blood mononuclear cell neutralization assay, a pseudovirus/TZM-bl neutralization assay or by assays for antibody-dependent cellular cytotoxicity (ADCC) were not significantly boosted. In contrast, T-cell proliferative responses to subtype B MN antigen and IFN-γ ELISpot responses to Env peptides were significantly enhanced. Four volunteers not primed with HIV-DNA and HIV-MVA before the CN54rgp140/GLA-AF immunizations mounted an antibody response, while cell-mediated responses were rare. After the two Env subtype C protein immunizations, a trend towards higher median subtype C Env binding antibody titers was found in vaccinees who had received HIV-DNA and HIV-MVA prior to the two Env protein immunizations as compared to unprimed vaccinees (p = 0.07). CONCLUSION: We report excellent tolerability, enhanced binding antibody responses and Env-specific cell-mediated immune responses but no ADCC antibody increase after two immunizations with a subtype C rgp140 protein adjuvanted in GLA-AF in healthy volunteers previously immunized with HIV-DNA and HIV-MVA. TRIAL REGISTRATION: International Clinical Trials Registry PACTR2010050002122368
format Online
Article
Text
id pubmed-4871571
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-48715712016-05-31 Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial Joachim, Agricola Bauer, Asli Joseph, Sarah Geldmacher, Christof Munseri, Patricia J. Aboud, Said Missanga, Marco Mann, Philipp Wahren, Britta Ferrari, Guido Polonis, Victoria R. Robb, Merlin L. Weber, Jonathan Tatoud, Roger Maboko, Leonard Hoelscher, Michael Lyamuya, Eligius F. Biberfeld, Gunnel Sandström, Eric Kroidl, Arne Bakari, Muhammad Nilsson, Charlotta McCormack, Sheena PLoS One Research Article BACKGROUND: A vaccine against HIV is widely considered the most effective and sustainable way of reducing new infections. We evaluated the safety and impact of boosting with subtype C CN54rgp140 envelope protein adjuvanted in glucopyranosyl lipid adjuvant (GLA-AF) in Tanzanian volunteers previously given three immunizations with HIV-DNA followed by two immunizations with recombinant modified vaccinia virus Ankara (HIV-MVA). METHODS: Forty volunteers (35 vaccinees and five placebo recipients) were given two CN54rgp140/GLA-AF immunizations 30–71 weeks after the last HIV-MVA vaccination. These immunizations were delivered intramuscularly four weeks apart. RESULTS: The vaccine was safe and well tolerated except for one episode of asymptomatic hypoglycaemia that was classified as severe adverse event. Two weeks after the second HIV-MVA vaccination 34 (97%) of the 35 previously vaccinated developed Env-specific binding antibodies, and 79% and 84% displayed IFN-γ ELISpot responses to Gag and Env, respectively. Binding antibodies to subtype C Env (included in HIV-DNA and protein boost), subtype B Env (included only in HIV-DNA) and CRF01_AE Env (included only in HIV-MVA) were significantly boosted by the CN54rgp140/GLA-AF immunizations. Functional antibodies detected using an infectious molecular clone virus/peripheral blood mononuclear cell neutralization assay, a pseudovirus/TZM-bl neutralization assay or by assays for antibody-dependent cellular cytotoxicity (ADCC) were not significantly boosted. In contrast, T-cell proliferative responses to subtype B MN antigen and IFN-γ ELISpot responses to Env peptides were significantly enhanced. Four volunteers not primed with HIV-DNA and HIV-MVA before the CN54rgp140/GLA-AF immunizations mounted an antibody response, while cell-mediated responses were rare. After the two Env subtype C protein immunizations, a trend towards higher median subtype C Env binding antibody titers was found in vaccinees who had received HIV-DNA and HIV-MVA prior to the two Env protein immunizations as compared to unprimed vaccinees (p = 0.07). CONCLUSION: We report excellent tolerability, enhanced binding antibody responses and Env-specific cell-mediated immune responses but no ADCC antibody increase after two immunizations with a subtype C rgp140 protein adjuvanted in GLA-AF in healthy volunteers previously immunized with HIV-DNA and HIV-MVA. TRIAL REGISTRATION: International Clinical Trials Registry PACTR2010050002122368 Public Library of Science 2016-05-18 /pmc/articles/PMC4871571/ /pubmed/27192151 http://dx.doi.org/10.1371/journal.pone.0155702 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Joachim, Agricola
Bauer, Asli
Joseph, Sarah
Geldmacher, Christof
Munseri, Patricia J.
Aboud, Said
Missanga, Marco
Mann, Philipp
Wahren, Britta
Ferrari, Guido
Polonis, Victoria R.
Robb, Merlin L.
Weber, Jonathan
Tatoud, Roger
Maboko, Leonard
Hoelscher, Michael
Lyamuya, Eligius F.
Biberfeld, Gunnel
Sandström, Eric
Kroidl, Arne
Bakari, Muhammad
Nilsson, Charlotta
McCormack, Sheena
Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title_full Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title_fullStr Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title_full_unstemmed Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title_short Boosting with Subtype C CN54rgp140 Protein Adjuvanted with Glucopyranosyl Lipid Adjuvant after Priming with HIV-DNA and HIV-MVA Is Safe and Enhances Immune Responses: A Phase I Trial
title_sort boosting with subtype c cn54rgp140 protein adjuvanted with glucopyranosyl lipid adjuvant after priming with hiv-dna and hiv-mva is safe and enhances immune responses: a phase i trial
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4871571/
https://www.ncbi.nlm.nih.gov/pubmed/27192151
http://dx.doi.org/10.1371/journal.pone.0155702
work_keys_str_mv AT joachimagricola boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT bauerasli boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT josephsarah boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT geldmacherchristof boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT munseripatriciaj boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT aboudsaid boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT missangamarco boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT mannphilipp boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT wahrenbritta boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT ferrariguido boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT polonisvictoriar boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT robbmerlinl boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT weberjonathan boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT tatoudroger boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT mabokoleonard boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT hoelschermichael boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT lyamuyaeligiusf boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT biberfeldgunnel boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT sandstromeric boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT kroidlarne boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT bakarimuhammad boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT nilssoncharlotta boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial
AT mccormacksheena boostingwithsubtypeccn54rgp140proteinadjuvantedwithglucopyranosyllipidadjuvantafterprimingwithhivdnaandhivmvaissafeandenhancesimmuneresponsesaphaseitrial

Ejemplares similares