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DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies

Successful future HIV vaccines are expected to generate an effective cellular and humoral response against the virus in both the peripheral blood and mucosal compartments. We previously reported the development of DNA-C and MVA-C vaccines based on HIV-1 subtype C and demonstrated their immunogenicit...

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Autores principales: Chege, Gerald K., Burgers, Wendy A., Müller, Tracey L., Gray, Clive M., Shephard, Enid G., Barnett, Susan W., Ferrari, Guido, Montefiori, David, Williamson, Carolyn, Williamson, Anna-Lise
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5287223/
https://www.ncbi.nlm.nih.gov/pubmed/28069361
http://dx.doi.org/10.1016/j.vaccine.2016.12.060
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author Chege, Gerald K.
Burgers, Wendy A.
Müller, Tracey L.
Gray, Clive M.
Shephard, Enid G.
Barnett, Susan W.
Ferrari, Guido
Montefiori, David
Williamson, Carolyn
Williamson, Anna-Lise
author_facet Chege, Gerald K.
Burgers, Wendy A.
Müller, Tracey L.
Gray, Clive M.
Shephard, Enid G.
Barnett, Susan W.
Ferrari, Guido
Montefiori, David
Williamson, Carolyn
Williamson, Anna-Lise
author_sort Chege, Gerald K.
collection PubMed
description Successful future HIV vaccines are expected to generate an effective cellular and humoral response against the virus in both the peripheral blood and mucosal compartments. We previously reported the development of DNA-C and MVA-C vaccines based on HIV-1 subtype C and demonstrated their immunogenicity when given in a DNA prime-MVA boost combination in a nonhuman primate model. In the current study, rhesus macaques previously vaccinated with a DNA-C and MVA-C vaccine regimen were re-vaccinated 3.5 years later with MVA-C followed by a protein vaccine based on HIV-1 subtype C envelope formulated with MF59 adjuvant (gp140Env/MF59), and finally a concurrent boost with both vaccines. A single MVA-C re-vaccination elicited T cell responses in all animals similar to previous peak responses, with 4/7 demonstrating responses >1000 SFU/10(6) PBMC. In contrast to an Env/MF59-only vaccine, concurrent boosting with MVA-C and Env/MF59 induced HIV-specific cellular responses in multiple mucosal associated lymph nodes in 6/7 animals, with high magnitude responses in some animals. Both vaccine regimens induced high titer Env-specific antibodies with ADCC activity, as well as neutralization of Tier 1 viruses and modest Tier 2 neutralization. These data demonstrate the feasibility of inducing HIV-specific immunity in the blood and mucosal sites of viral entry by means of DNA and poxvirus-vectored vaccines, in combination with a HIV envelope-based protein vaccine.
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spelling pubmed-52872232017-02-07 DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies Chege, Gerald K. Burgers, Wendy A. Müller, Tracey L. Gray, Clive M. Shephard, Enid G. Barnett, Susan W. Ferrari, Guido Montefiori, David Williamson, Carolyn Williamson, Anna-Lise Vaccine Article Successful future HIV vaccines are expected to generate an effective cellular and humoral response against the virus in both the peripheral blood and mucosal compartments. We previously reported the development of DNA-C and MVA-C vaccines based on HIV-1 subtype C and demonstrated their immunogenicity when given in a DNA prime-MVA boost combination in a nonhuman primate model. In the current study, rhesus macaques previously vaccinated with a DNA-C and MVA-C vaccine regimen were re-vaccinated 3.5 years later with MVA-C followed by a protein vaccine based on HIV-1 subtype C envelope formulated with MF59 adjuvant (gp140Env/MF59), and finally a concurrent boost with both vaccines. A single MVA-C re-vaccination elicited T cell responses in all animals similar to previous peak responses, with 4/7 demonstrating responses >1000 SFU/10(6) PBMC. In contrast to an Env/MF59-only vaccine, concurrent boosting with MVA-C and Env/MF59 induced HIV-specific cellular responses in multiple mucosal associated lymph nodes in 6/7 animals, with high magnitude responses in some animals. Both vaccine regimens induced high titer Env-specific antibodies with ADCC activity, as well as neutralization of Tier 1 viruses and modest Tier 2 neutralization. These data demonstrate the feasibility of inducing HIV-specific immunity in the blood and mucosal sites of viral entry by means of DNA and poxvirus-vectored vaccines, in combination with a HIV envelope-based protein vaccine. Elsevier Science 2017-02-07 /pmc/articles/PMC5287223/ /pubmed/28069361 http://dx.doi.org/10.1016/j.vaccine.2016.12.060 Text en © 2017 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Chege, Gerald K.
Burgers, Wendy A.
Müller, Tracey L.
Gray, Clive M.
Shephard, Enid G.
Barnett, Susan W.
Ferrari, Guido
Montefiori, David
Williamson, Carolyn
Williamson, Anna-Lise
DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title_full DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title_fullStr DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title_full_unstemmed DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title_short DNA-MVA-protein vaccination of rhesus macaques induces HIV-specific immunity in mucosal-associated lymph nodes and functional antibodies
title_sort dna-mva-protein vaccination of rhesus macaques induces hiv-specific immunity in mucosal-associated lymph nodes and functional antibodies
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5287223/
https://www.ncbi.nlm.nih.gov/pubmed/28069361
http://dx.doi.org/10.1016/j.vaccine.2016.12.060
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