Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection

There is increasing evidence for the importance of human leukocyte antigen C (HLA-C)-restricted CD8(+) T cells in HIV-1 control, but these responses are relatively poorly investigated. The number of HLA-C-restricted HIV-1 epitopes identified is much smaller than those of HLA-A-restricted or HLA-B-re...

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Autores principales: Chikata, Takayuki, Paes, Wayne, Kuse, Nozomi, Partridge, Thomas, Gatanaga, Hiroyuki, Zhang, Yu, Kuroki, Kimiko, Maenaka, Katsumi, Ternette, Nicola, Oka, Shinichi, Borrow, Persephone, Takiguchi, Masafumi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2022
Materias:
Pathogenesis and Immunity
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9131871/
https://www.ncbi.nlm.nih.gov/pubmed/35475667
http://dx.doi.org/10.1128/jvi.00432-22
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author Chikata, Takayuki
Paes, Wayne
Kuse, Nozomi
Partridge, Thomas
Gatanaga, Hiroyuki
Zhang, Yu
Kuroki, Kimiko
Maenaka, Katsumi
Ternette, Nicola
Oka, Shinichi
Borrow, Persephone
Takiguchi, Masafumi
author_facet Chikata, Takayuki
Paes, Wayne
Kuse, Nozomi
Partridge, Thomas
Gatanaga, Hiroyuki
Zhang, Yu
Kuroki, Kimiko
Maenaka, Katsumi
Ternette, Nicola
Oka, Shinichi
Borrow, Persephone
Takiguchi, Masafumi
author_sort Chikata, Takayuki
collection PubMed
description There is increasing evidence for the importance of human leukocyte antigen C (HLA-C)-restricted CD8(+) T cells in HIV-1 control, but these responses are relatively poorly investigated. The number of HLA-C-restricted HIV-1 epitopes identified is much smaller than those of HLA-A-restricted or HLA-B-restricted ones. Here, we utilized a mass spectrometry-based approach to identify HIV-1 peptides presented by HLA-C*14:03 protective and HLA-C*14:02 nonprotective alleles. We identified 25 8- to 11-mer HLA-I-bound HIV-1 peptides from HIV-1-infected HLA-C*14:02(+)/14:03(+) cells. Analysis of T cell responses to these peptides identified novel 6 T cell epitopes targeted in HIV-1-infected HLA-C*14:02(+)/14:03(+) subjects. Analyses using HLA stabilization assays demonstrated that all 6 epitope peptides exhibited higher binding to and greater cell surface stabilization of HLA-C*14:02 than HLA-C*14:03. T cell response magnitudes were typically higher in HLA-C*14:02(+) than HLA-C*14:03(+) individuals, with responses to the Pol KM9 and Nef epitopes being significantly higher. The results show that HLA-C*14:02 can elicit stronger T cell responses to HIV-1 than HLA-C*14:03 and suggest that the single amino acid difference between these HLA-C14 subtypes at position 21, outside the peptide-binding groove, indirectly influences the stability of peptide-HLA-C*14 complexes and induction/expansion of HIV-specific T cells. Taken together with a previous finding that KIR2DL2(+) NK cells recognized HLA-C*14:03(+) HIV-1-infected cells more than HLA-C*14:02(+) ones, the present study indicates that these HLA-C*14 subtypes differentially impact HIV-1 control by T cells and NK cells. IMPORTANCE Some human leukocyte antigen (HLA) class I alleles are associated with good clinical outcomes in HIV-1 infection and are called protective HLA alleles. Identification of T cell epitopes restricted by protective HLA alleles can give important insight into virus-immune system interactions and inform design of immune-based prophylactic/therapeutic strategies. Although epitopes restricted by many protective HLA-A/B alleles have been identified, protective HLA-C alleles are relatively understudied. Here, we identified 6 novel T cell epitopes presented by both HLA-C*14:02 (no association with protection) and HLA-C*14:03 (protective) using a mass spectrometry-based immunopeptidome profiling approach. We found that these peptides bound to and stabilized HLA-C*14:02 better than HLA-C*14:03 and observed differences in induction/expansion of epitope-specific T cell responses in HIV-infected HLA-C*14:02(+) versus HLA-C*14:03(+) individuals. These results enhance understanding of how the microstructural difference at position 21 between these HLA-C*14 subtypes may influence cellular immune responses involved in viral control in HIV-1 infection.
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spelling pubmed-91318712022-05-26 Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection Chikata, Takayuki Paes, Wayne Kuse, Nozomi Partridge, Thomas Gatanaga, Hiroyuki Zhang, Yu Kuroki, Kimiko Maenaka, Katsumi Ternette, Nicola Oka, Shinichi Borrow, Persephone Takiguchi, Masafumi J Virol Pathogenesis and Immunity There is increasing evidence for the importance of human leukocyte antigen C (HLA-C)-restricted CD8(+) T cells in HIV-1 control, but these responses are relatively poorly investigated. The number of HLA-C-restricted HIV-1 epitopes identified is much smaller than those of HLA-A-restricted or HLA-B-restricted ones. Here, we utilized a mass spectrometry-based approach to identify HIV-1 peptides presented by HLA-C*14:03 protective and HLA-C*14:02 nonprotective alleles. We identified 25 8- to 11-mer HLA-I-bound HIV-1 peptides from HIV-1-infected HLA-C*14:02(+)/14:03(+) cells. Analysis of T cell responses to these peptides identified novel 6 T cell epitopes targeted in HIV-1-infected HLA-C*14:02(+)/14:03(+) subjects. Analyses using HLA stabilization assays demonstrated that all 6 epitope peptides exhibited higher binding to and greater cell surface stabilization of HLA-C*14:02 than HLA-C*14:03. T cell response magnitudes were typically higher in HLA-C*14:02(+) than HLA-C*14:03(+) individuals, with responses to the Pol KM9 and Nef epitopes being significantly higher. The results show that HLA-C*14:02 can elicit stronger T cell responses to HIV-1 than HLA-C*14:03 and suggest that the single amino acid difference between these HLA-C14 subtypes at position 21, outside the peptide-binding groove, indirectly influences the stability of peptide-HLA-C*14 complexes and induction/expansion of HIV-specific T cells. Taken together with a previous finding that KIR2DL2(+) NK cells recognized HLA-C*14:03(+) HIV-1-infected cells more than HLA-C*14:02(+) ones, the present study indicates that these HLA-C*14 subtypes differentially impact HIV-1 control by T cells and NK cells. IMPORTANCE Some human leukocyte antigen (HLA) class I alleles are associated with good clinical outcomes in HIV-1 infection and are called protective HLA alleles. Identification of T cell epitopes restricted by protective HLA alleles can give important insight into virus-immune system interactions and inform design of immune-based prophylactic/therapeutic strategies. Although epitopes restricted by many protective HLA-A/B alleles have been identified, protective HLA-C alleles are relatively understudied. Here, we identified 6 novel T cell epitopes presented by both HLA-C*14:02 (no association with protection) and HLA-C*14:03 (protective) using a mass spectrometry-based immunopeptidome profiling approach. We found that these peptides bound to and stabilized HLA-C*14:02 better than HLA-C*14:03 and observed differences in induction/expansion of epitope-specific T cell responses in HIV-infected HLA-C*14:02(+) versus HLA-C*14:03(+) individuals. These results enhance understanding of how the microstructural difference at position 21 between these HLA-C*14 subtypes may influence cellular immune responses involved in viral control in HIV-1 infection. American Society for Microbiology 2022-04-27 /pmc/articles/PMC9131871/ /pubmed/35475667 http://dx.doi.org/10.1128/jvi.00432-22 Text en Copyright © 2022 Chikata et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Pathogenesis and Immunity
Chikata, Takayuki
Paes, Wayne
Kuse, Nozomi
Partridge, Thomas
Gatanaga, Hiroyuki
Zhang, Yu
Kuroki, Kimiko
Maenaka, Katsumi
Ternette, Nicola
Oka, Shinichi
Borrow, Persephone
Takiguchi, Masafumi
Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title_full Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title_fullStr Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title_full_unstemmed Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title_short Impact of Micropolymorphism Outside the Peptide Binding Groove in the Clinically Relevant Allele HLA-C*14 on T Cell Responses in HIV-1 Infection
title_sort impact of micropolymorphism outside the peptide binding groove in the clinically relevant allele hla-c*14 on t cell responses in hiv-1 infection
topic Pathogenesis and Immunity
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9131871/
https://www.ncbi.nlm.nih.gov/pubmed/35475667
http://dx.doi.org/10.1128/jvi.00432-22
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