Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth

A vaccine will likely be one of the key tools for ending the HIV-1/AIDS epidemic by preventing HIV-1 spread within uninfected populations and achieving a cure for people living with HIV-1. The currently prevailing view of the vaccine field is to introduce protective antibodies, nevertheless, a vacci...

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Autores principales: Moyo, Nathifa, Wee, Edmund G., Korber, Bette, Bahl, Kapil, Falcone, Samantha, Himansu, Sunny, Wong, Adrianne L., Dey, Antu K., Feinberg, Mark, Hanke, Tomáš
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Communication
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7563622/
https://www.ncbi.nlm.nih.gov/pubmed/32640600
http://dx.doi.org/10.3390/vaccines8030360
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author Moyo, Nathifa
Wee, Edmund G.
Korber, Bette
Bahl, Kapil
Falcone, Samantha
Himansu, Sunny
Wong, Adrianne L.
Dey, Antu K.
Feinberg, Mark
Hanke, Tomáš
author_facet Moyo, Nathifa
Wee, Edmund G.
Korber, Bette
Bahl, Kapil
Falcone, Samantha
Himansu, Sunny
Wong, Adrianne L.
Dey, Antu K.
Feinberg, Mark
Hanke, Tomáš
author_sort Moyo, Nathifa
collection PubMed
description A vaccine will likely be one of the key tools for ending the HIV-1/AIDS epidemic by preventing HIV-1 spread within uninfected populations and achieving a cure for people living with HIV-1. The currently prevailing view of the vaccine field is to introduce protective antibodies, nevertheless, a vaccine to be effective may need to harness protective T cells. We postulated that focusing a T-cell response on the most vulnerable regions of the HIV-1 proteome while maximizing a perfect match between the vaccine and circulating viruses will control HIV-1 replication. We currently use a combination of replication-deficient simian (chimpanzee) adenovirus and poxvirus modified vaccinia virus Ankara to deliver bivalent conserved-mosaic immunogens to human volunteers. Here, we exploit the mRNA platform by designing tetravalent immunogens designated as HIVconsvM, and demonstrate that mRNA formulated in lipid nanoparticles induces potent, broad and polyfunctional T-cell responses in a pre-clinical model. These results support optimization and further development of this vaccine strategy in experimental medicine trials in humans.
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spelling pubmed-75636222020-10-27 Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth Moyo, Nathifa Wee, Edmund G. Korber, Bette Bahl, Kapil Falcone, Samantha Himansu, Sunny Wong, Adrianne L. Dey, Antu K. Feinberg, Mark Hanke, Tomáš Vaccines (Basel) Communication A vaccine will likely be one of the key tools for ending the HIV-1/AIDS epidemic by preventing HIV-1 spread within uninfected populations and achieving a cure for people living with HIV-1. The currently prevailing view of the vaccine field is to introduce protective antibodies, nevertheless, a vaccine to be effective may need to harness protective T cells. We postulated that focusing a T-cell response on the most vulnerable regions of the HIV-1 proteome while maximizing a perfect match between the vaccine and circulating viruses will control HIV-1 replication. We currently use a combination of replication-deficient simian (chimpanzee) adenovirus and poxvirus modified vaccinia virus Ankara to deliver bivalent conserved-mosaic immunogens to human volunteers. Here, we exploit the mRNA platform by designing tetravalent immunogens designated as HIVconsvM, and demonstrate that mRNA formulated in lipid nanoparticles induces potent, broad and polyfunctional T-cell responses in a pre-clinical model. These results support optimization and further development of this vaccine strategy in experimental medicine trials in humans. MDPI 2020-07-06 /pmc/articles/PMC7563622/ /pubmed/32640600 http://dx.doi.org/10.3390/vaccines8030360 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Communication
Moyo, Nathifa
Wee, Edmund G.
Korber, Bette
Bahl, Kapil
Falcone, Samantha
Himansu, Sunny
Wong, Adrianne L.
Dey, Antu K.
Feinberg, Mark
Hanke, Tomáš
Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title_full Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title_fullStr Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title_full_unstemmed Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title_short Tetravalent Immunogen Assembled from Conserved Regions of HIV-1 and Delivered as mRNA Demonstrates Potent Preclinical T-Cell Immunogenicity and Breadth
title_sort tetravalent immunogen assembled from conserved regions of hiv-1 and delivered as mrna demonstrates potent preclinical t-cell immunogenicity and breadth
topic Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7563622/
https://www.ncbi.nlm.nih.gov/pubmed/32640600
http://dx.doi.org/10.3390/vaccines8030360
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