Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design

A successful HIV vaccine will likely induce both humoral and cell-mediated immunity, however, the enormous diversity of HIV has hampered the development of a vaccine that effectively elicits both arms of the adaptive immune response. To tackle the problem of viral diversity, T cell-based vaccine app...

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Autores principales: Kunwar, Pratima, Hawkins, Natalie, Dinges, Warren L., Liu, Yi, Gabriel, Erin E., Swan, David A., Stevens, Claire E., Maenza, Janine, Collier, Ann C., Mullins, James I., Hertz, Tomer, Yu, Xuesong, Horton, Helen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3669284/
https://www.ncbi.nlm.nih.gov/pubmed/23741326
http://dx.doi.org/10.1371/journal.pone.0064405
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author Kunwar, Pratima
Hawkins, Natalie
Dinges, Warren L.
Liu, Yi
Gabriel, Erin E.
Swan, David A.
Stevens, Claire E.
Maenza, Janine
Collier, Ann C.
Mullins, James I.
Hertz, Tomer
Yu, Xuesong
Horton, Helen
author_facet Kunwar, Pratima
Hawkins, Natalie
Dinges, Warren L.
Liu, Yi
Gabriel, Erin E.
Swan, David A.
Stevens, Claire E.
Maenza, Janine
Collier, Ann C.
Mullins, James I.
Hertz, Tomer
Yu, Xuesong
Horton, Helen
author_sort Kunwar, Pratima
collection PubMed
description A successful HIV vaccine will likely induce both humoral and cell-mediated immunity, however, the enormous diversity of HIV has hampered the development of a vaccine that effectively elicits both arms of the adaptive immune response. To tackle the problem of viral diversity, T cell-based vaccine approaches have focused on two main strategies (i) increasing the breadth of vaccine-induced responses or (ii) increasing vaccine-induced responses targeting only conserved regions of the virus. The relative extent to which set-point viremia is impacted by epitope-conservation of CD8(+) T cell responses elicited during early HIV-infection is unknown but has important implications for vaccine design. To address this question, we comprehensively mapped HIV-1 CD8(+) T cell epitope-specificities in 23 ART-naïve individuals during early infection and computed their conservation score (CS) by three different methods (prevalence, entropy and conseq) on clade-B and group-M sequence alignments. The majority of CD8(+) T cell responses were directed against variable epitopes (p<0.01). Interestingly, increasing breadth of CD8(+) T cell responses specifically recognizing conserved epitopes was associated with lower set-point viremia (r = - 0.65, p = 0.009). Moreover, subjects possessing CD8(+) T cells recognizing at least one conserved epitope had 1.4 log(10) lower set-point viremia compared to those recognizing only variable epitopes (p = 0.021). The association between viral control and the breadth of conserved CD8(+) T cell responses may be influenced by the method of CS definition and sequences used to determine conservation levels. Strikingly, targeting variable versus conserved epitopes was independent of HLA type (p = 0.215). The associations with viral control were independent of functional avidity of CD8(+) T cell responses elicited during early infection. Taken together, these data suggest that the next-generation of T-cell based HIV-1 vaccines should focus on strategies that can elicit CD8(+) T cell responses to multiple conserved epitopes of HIV-1.
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spelling pubmed-36692842013-06-05 Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design Kunwar, Pratima Hawkins, Natalie Dinges, Warren L. Liu, Yi Gabriel, Erin E. Swan, David A. Stevens, Claire E. Maenza, Janine Collier, Ann C. Mullins, James I. Hertz, Tomer Yu, Xuesong Horton, Helen PLoS One Research Article A successful HIV vaccine will likely induce both humoral and cell-mediated immunity, however, the enormous diversity of HIV has hampered the development of a vaccine that effectively elicits both arms of the adaptive immune response. To tackle the problem of viral diversity, T cell-based vaccine approaches have focused on two main strategies (i) increasing the breadth of vaccine-induced responses or (ii) increasing vaccine-induced responses targeting only conserved regions of the virus. The relative extent to which set-point viremia is impacted by epitope-conservation of CD8(+) T cell responses elicited during early HIV-infection is unknown but has important implications for vaccine design. To address this question, we comprehensively mapped HIV-1 CD8(+) T cell epitope-specificities in 23 ART-naïve individuals during early infection and computed their conservation score (CS) by three different methods (prevalence, entropy and conseq) on clade-B and group-M sequence alignments. The majority of CD8(+) T cell responses were directed against variable epitopes (p<0.01). Interestingly, increasing breadth of CD8(+) T cell responses specifically recognizing conserved epitopes was associated with lower set-point viremia (r = - 0.65, p = 0.009). Moreover, subjects possessing CD8(+) T cells recognizing at least one conserved epitope had 1.4 log(10) lower set-point viremia compared to those recognizing only variable epitopes (p = 0.021). The association between viral control and the breadth of conserved CD8(+) T cell responses may be influenced by the method of CS definition and sequences used to determine conservation levels. Strikingly, targeting variable versus conserved epitopes was independent of HLA type (p = 0.215). The associations with viral control were independent of functional avidity of CD8(+) T cell responses elicited during early infection. Taken together, these data suggest that the next-generation of T-cell based HIV-1 vaccines should focus on strategies that can elicit CD8(+) T cell responses to multiple conserved epitopes of HIV-1. Public Library of Science 2013-05-31 /pmc/articles/PMC3669284/ /pubmed/23741326 http://dx.doi.org/10.1371/journal.pone.0064405 Text en © 2013 Kunwar 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
Kunwar, Pratima
Hawkins, Natalie
Dinges, Warren L.
Liu, Yi
Gabriel, Erin E.
Swan, David A.
Stevens, Claire E.
Maenza, Janine
Collier, Ann C.
Mullins, James I.
Hertz, Tomer
Yu, Xuesong
Horton, Helen
Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title_full Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title_fullStr Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title_full_unstemmed Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title_short Superior Control of HIV-1 Replication by CD8+ T Cells Targeting Conserved Epitopes: Implications for HIV Vaccine Design
title_sort superior control of hiv-1 replication by cd8+ t cells targeting conserved epitopes: implications for hiv vaccine design
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3669284/
https://www.ncbi.nlm.nih.gov/pubmed/23741326
http://dx.doi.org/10.1371/journal.pone.0064405
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