CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response

BACKGROUND: Subtype A is a major strain in the HIV-1 pandemic in eastern Europe, central Asia and in certain regions of east Africa, notably in rural Kenya. While considerable effort has been focused upon mapping and defining immunodominant CTL epitopes in HIV-1 subtype B and subtype C infections, f...

Descripción completa

Detalles Bibliográficos
Autores principales: Currier, Jeffrey R, Visawapoka, Unchalee, Tovanabutra, Sodsai, Mason, Carl J, Birx, Deborah L, McCutchan, Francine E, Cox, Josephine H
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1464141/
https://www.ncbi.nlm.nih.gov/pubmed/16620386
http://dx.doi.org/10.1186/1471-2172-7-8
_version_ 1782127542127296512
author Currier, Jeffrey R
Visawapoka, Unchalee
Tovanabutra, Sodsai
Mason, Carl J
Birx, Deborah L
McCutchan, Francine E
Cox, Josephine H
author_facet Currier, Jeffrey R
Visawapoka, Unchalee
Tovanabutra, Sodsai
Mason, Carl J
Birx, Deborah L
McCutchan, Francine E
Cox, Josephine H
author_sort Currier, Jeffrey R
collection PubMed
description BACKGROUND: Subtype A is a major strain in the HIV-1 pandemic in eastern Europe, central Asia and in certain regions of east Africa, notably in rural Kenya. While considerable effort has been focused upon mapping and defining immunodominant CTL epitopes in HIV-1 subtype B and subtype C infections, few epitope mapping studies have focused upon subtype A. RESULTS: We have used the IFN-γ ELIspot assay and overlapping peptide pools to show that the pattern of CTL recognition of the Gag and Nef proteins in subtype A infection is similar to that seen in subtypes B and C. The p17 and p24 proteins of Gag and the central conserved region of Nef were targeted by CTL from HIV-1-infected Kenyans. Several epitope/HLA associations commonly seen in subtype B and C infection were also observed in subtype A infections. Notably, an immunodominant HLA-C restricted epitope (Gag 296–304; YL9) was observed, with 8/9 HLA-C(W)0304 subjects responding to this epitope. Screening the cohort with peptide sets representing subtypes A, C and D (the three most prevalent HIV-1 subtypes in east Africa), revealed that peptide sets based upon an homologous subtype (either isolate or consensus) only marginally improved the capacity to detect CTL responses. While the different peptide sets detected a similar number of responses (particularly in the Gag protein), each set was capable of detecting unique responses not identified with the other peptide sets. CONCLUSION: Hence, screening with multiple peptide sets representing different sequences, and by extension different epitope variants, can increase the detectable breadth of the HIV-1-specific CTL response. Interpreting the true extent of cross-reactivity may be hampered by the use of 15-mer peptides at a single concentration and a lack of knowledge of the sequence that primed any given CTL response. Therefore, reagent choice and knowledge of the exact sequences that prime CTL responses will be important factors in experimentally defining cross-reactive CTL responses and their role in HIV-1 disease pathogenesis and validating vaccines aimed at generating broadly cross-reactive CTL responses.
format Text
id pubmed-1464141
institution National Center for Biotechnology Information
language English
publishDate 2006
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-14641412006-05-23 CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response Currier, Jeffrey R Visawapoka, Unchalee Tovanabutra, Sodsai Mason, Carl J Birx, Deborah L McCutchan, Francine E Cox, Josephine H BMC Immunol Research Article BACKGROUND: Subtype A is a major strain in the HIV-1 pandemic in eastern Europe, central Asia and in certain regions of east Africa, notably in rural Kenya. While considerable effort has been focused upon mapping and defining immunodominant CTL epitopes in HIV-1 subtype B and subtype C infections, few epitope mapping studies have focused upon subtype A. RESULTS: We have used the IFN-γ ELIspot assay and overlapping peptide pools to show that the pattern of CTL recognition of the Gag and Nef proteins in subtype A infection is similar to that seen in subtypes B and C. The p17 and p24 proteins of Gag and the central conserved region of Nef were targeted by CTL from HIV-1-infected Kenyans. Several epitope/HLA associations commonly seen in subtype B and C infection were also observed in subtype A infections. Notably, an immunodominant HLA-C restricted epitope (Gag 296–304; YL9) was observed, with 8/9 HLA-C(W)0304 subjects responding to this epitope. Screening the cohort with peptide sets representing subtypes A, C and D (the three most prevalent HIV-1 subtypes in east Africa), revealed that peptide sets based upon an homologous subtype (either isolate or consensus) only marginally improved the capacity to detect CTL responses. While the different peptide sets detected a similar number of responses (particularly in the Gag protein), each set was capable of detecting unique responses not identified with the other peptide sets. CONCLUSION: Hence, screening with multiple peptide sets representing different sequences, and by extension different epitope variants, can increase the detectable breadth of the HIV-1-specific CTL response. Interpreting the true extent of cross-reactivity may be hampered by the use of 15-mer peptides at a single concentration and a lack of knowledge of the sequence that primed any given CTL response. Therefore, reagent choice and knowledge of the exact sequences that prime CTL responses will be important factors in experimentally defining cross-reactive CTL responses and their role in HIV-1 disease pathogenesis and validating vaccines aimed at generating broadly cross-reactive CTL responses. BioMed Central 2006-04-18 /pmc/articles/PMC1464141/ /pubmed/16620386 http://dx.doi.org/10.1186/1471-2172-7-8 Text en Copyright © 2006 Currier et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Currier, Jeffrey R
Visawapoka, Unchalee
Tovanabutra, Sodsai
Mason, Carl J
Birx, Deborah L
McCutchan, Francine E
Cox, Josephine H
CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title_full CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title_fullStr CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title_full_unstemmed CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title_short CTL epitope distribution patterns in the Gag and Nef proteins of HIV-1 from subtype A infected subjects in Kenya: Use of multiple peptide sets increases the detectable breadth of the CTL response
title_sort ctl epitope distribution patterns in the gag and nef proteins of hiv-1 from subtype a infected subjects in kenya: use of multiple peptide sets increases the detectable breadth of the ctl response
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1464141/
https://www.ncbi.nlm.nih.gov/pubmed/16620386
http://dx.doi.org/10.1186/1471-2172-7-8
work_keys_str_mv AT currierjeffreyr ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT visawapokaunchalee ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT tovanabutrasodsai ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT masoncarlj ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT birxdeborahl ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT mccutchanfrancinee ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse
AT coxjosephineh ctlepitopedistributionpatternsinthegagandnefproteinsofhiv1fromsubtypeainfectedsubjectsinkenyauseofmultiplepeptidesetsincreasesthedetectablebreadthofthectlresponse

Ejemplares similares