Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses

BACKGROUND: High mutation rates of human immunodeficiency virus (HIV) allows escape from T cell recognition preventing development of effective T cell vaccines. Vaccines that induce diverse T cell immune responses would help overcome this problem. Using SIV gag as a model vaccine, we investigated tw...

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Autores principales: Benlahrech, Adel, Meiser, Andrea, Herath, Shanthi, Papagatsias, Timos, Athanasopoulos, Takis, Li, Fucheng, Self, Steve, Bachy, Veronique, Hervouet, Catherine, Logan, Karen, Klavinskis, Linda, Dickson, George, Patterson, Steven
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3485275/
https://www.ncbi.nlm.nih.gov/pubmed/23118924
http://dx.doi.org/10.1371/journal.pone.0048038
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author Benlahrech, Adel
Meiser, Andrea
Herath, Shanthi
Papagatsias, Timos
Athanasopoulos, Takis
Li, Fucheng
Self, Steve
Bachy, Veronique
Hervouet, Catherine
Logan, Karen
Klavinskis, Linda
Dickson, George
Patterson, Steven
author_facet Benlahrech, Adel
Meiser, Andrea
Herath, Shanthi
Papagatsias, Timos
Athanasopoulos, Takis
Li, Fucheng
Self, Steve
Bachy, Veronique
Hervouet, Catherine
Logan, Karen
Klavinskis, Linda
Dickson, George
Patterson, Steven
author_sort Benlahrech, Adel
collection PubMed
description BACKGROUND: High mutation rates of human immunodeficiency virus (HIV) allows escape from T cell recognition preventing development of effective T cell vaccines. Vaccines that induce diverse T cell immune responses would help overcome this problem. Using SIV gag as a model vaccine, we investigated two approaches to increase the breadth of the CD8 T cell response. Namely, fusion of vaccine genes to ubiquitin to target the proteasome and increase levels of MHC class I peptide complexes and gene fragmentation to overcome competition between epitopes for presentation and recognition. METHODOLOGY/PRINCIPAL FINDINGS: Three vaccines were compared: full-length unmodified SIV-mac239 gag, full-length gag fused at the N-terminus to ubiquitin and 7 gag fragments of equal size spanning the whole of gag with ubiquitin-fused to the N-terminus of each fragment. Genes were cloned into a replication defective adenovirus vector and immunogenicity assessed in an in vitro human priming system. The breadth of the CD8 T cell response, defined by the number of distinct epitopes, was assessed by IFN-γ-ELISPOT and memory phenotype and cytokine production evaluated by flow cytometry. We observed an increase of two- to six-fold in the number of epitopes recognised in the ubiquitin-fused fragments compared to the ubiquitin-fused full-length gag. In contrast, although proteasomal targeting was achieved, there was a marked reduction in the number of epitopes recognised in the ubiquitin-fused full-length gag compared to the full-length unmodified gene, but there were no differences in the number of epitope responses induced by non-ubiquitinated full-length gag and the ubiquitin-fused mini genes. Fragmentation and ubiquitination did not affect T cell memory differentiation and polyfunctionality, though most responses were directed against the Ad5 vector. CONCLUSION/SIGNIFICANCE: Fragmentation but not fusion with ubiquitin increases the breadth of the CD8 T vaccine response against SIV-mac239 gag. Thus gene fragmentation of HIV vaccines may maximise responses.
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spelling pubmed-34852752012-11-01 Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses Benlahrech, Adel Meiser, Andrea Herath, Shanthi Papagatsias, Timos Athanasopoulos, Takis Li, Fucheng Self, Steve Bachy, Veronique Hervouet, Catherine Logan, Karen Klavinskis, Linda Dickson, George Patterson, Steven PLoS One Research Article BACKGROUND: High mutation rates of human immunodeficiency virus (HIV) allows escape from T cell recognition preventing development of effective T cell vaccines. Vaccines that induce diverse T cell immune responses would help overcome this problem. Using SIV gag as a model vaccine, we investigated two approaches to increase the breadth of the CD8 T cell response. Namely, fusion of vaccine genes to ubiquitin to target the proteasome and increase levels of MHC class I peptide complexes and gene fragmentation to overcome competition between epitopes for presentation and recognition. METHODOLOGY/PRINCIPAL FINDINGS: Three vaccines were compared: full-length unmodified SIV-mac239 gag, full-length gag fused at the N-terminus to ubiquitin and 7 gag fragments of equal size spanning the whole of gag with ubiquitin-fused to the N-terminus of each fragment. Genes were cloned into a replication defective adenovirus vector and immunogenicity assessed in an in vitro human priming system. The breadth of the CD8 T cell response, defined by the number of distinct epitopes, was assessed by IFN-γ-ELISPOT and memory phenotype and cytokine production evaluated by flow cytometry. We observed an increase of two- to six-fold in the number of epitopes recognised in the ubiquitin-fused fragments compared to the ubiquitin-fused full-length gag. In contrast, although proteasomal targeting was achieved, there was a marked reduction in the number of epitopes recognised in the ubiquitin-fused full-length gag compared to the full-length unmodified gene, but there were no differences in the number of epitope responses induced by non-ubiquitinated full-length gag and the ubiquitin-fused mini genes. Fragmentation and ubiquitination did not affect T cell memory differentiation and polyfunctionality, though most responses were directed against the Ad5 vector. CONCLUSION/SIGNIFICANCE: Fragmentation but not fusion with ubiquitin increases the breadth of the CD8 T vaccine response against SIV-mac239 gag. Thus gene fragmentation of HIV vaccines may maximise responses. Public Library of Science 2012-10-31 /pmc/articles/PMC3485275/ /pubmed/23118924 http://dx.doi.org/10.1371/journal.pone.0048038 Text en © 2012 Benlahrech et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Benlahrech, Adel
Meiser, Andrea
Herath, Shanthi
Papagatsias, Timos
Athanasopoulos, Takis
Li, Fucheng
Self, Steve
Bachy, Veronique
Hervouet, Catherine
Logan, Karen
Klavinskis, Linda
Dickson, George
Patterson, Steven
Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title_full Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title_fullStr Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title_full_unstemmed Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title_short Fragmentation of SIV-gag Vaccine Induces Broader T Cell Responses
title_sort fragmentation of siv-gag vaccine induces broader t cell responses
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3485275/
https://www.ncbi.nlm.nih.gov/pubmed/23118924
http://dx.doi.org/10.1371/journal.pone.0048038
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