Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01

CD8(+) CTL responses directed toward the HLA-B*51:01–restricted HIV-RT(128–135) epitope TAFTIPSI (TI8) are associated with long-term nonprogression to AIDS. Clonotypic analysis of responses to B51-TI8 revealed a public clonotype using TRAV17/TRBV7-3 TCR genes in six out of seven HLA-B*51:01(+) patie...

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Autores principales: Motozono, Chihiro, Kuse, Nozomi, Sun, Xiaoming, Rizkallah, Pierre J., Fuller, Anna, Oka, Shinichi, Cole, David K., Sewell, Andrew K., Takiguchi, Masafumi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: AAI 2014
Materias:
Molecular and Structural Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3962895/
https://www.ncbi.nlm.nih.gov/pubmed/24600035
http://dx.doi.org/10.4049/jimmunol.1302667
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author Motozono, Chihiro
Kuse, Nozomi
Sun, Xiaoming
Rizkallah, Pierre J.
Fuller, Anna
Oka, Shinichi
Cole, David K.
Sewell, Andrew K.
Takiguchi, Masafumi
author_facet Motozono, Chihiro
Kuse, Nozomi
Sun, Xiaoming
Rizkallah, Pierre J.
Fuller, Anna
Oka, Shinichi
Cole, David K.
Sewell, Andrew K.
Takiguchi, Masafumi
author_sort Motozono, Chihiro
collection PubMed
description CD8(+) CTL responses directed toward the HLA-B*51:01–restricted HIV-RT(128–135) epitope TAFTIPSI (TI8) are associated with long-term nonprogression to AIDS. Clonotypic analysis of responses to B51-TI8 revealed a public clonotype using TRAV17/TRBV7-3 TCR genes in six out of seven HLA-B*51:01(+) patients. Structural analysis of a TRAV17/TRBV7-3 TCR in complex with HLA–B51-TI8, to our knowledge the first human TCR complexed with an 8-mer peptide, explained this bias, as the unique combination of residues encoded by these genes was central to the interaction. The relatively featureless peptide-MHC (pMHC) was mainly recognized by the TCR CDR1 and CDR2 loops in an MHC-centric manner. A highly conserved residue Arg(97) in the CDR3α loop played a major role in recognition of peptide and MHC to form a stabilizing ball-and-socket interaction with the MHC and peptide, contributing to the selection of the public TCR clonotype. Surface plasmon resonance equilibrium binding analysis showed the low affinity of this public TCR is in accordance with the only other 8-mer interaction studied to date (murine 2C TCR–H-2K(b)-dEV8). Like pMHC class II complexes, 8-mer peptides do not protrude out the MHC class I binding groove like those of longer peptides. The accumulated evidence suggests that weak affinity might be a common characteristic of TCR binding to featureless pMHC landscapes.
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spelling pubmed-39628952014-03-24 Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01 Motozono, Chihiro Kuse, Nozomi Sun, Xiaoming Rizkallah, Pierre J. Fuller, Anna Oka, Shinichi Cole, David K. Sewell, Andrew K. Takiguchi, Masafumi J Immunol Molecular and Structural Immunology CD8(+) CTL responses directed toward the HLA-B*51:01–restricted HIV-RT(128–135) epitope TAFTIPSI (TI8) are associated with long-term nonprogression to AIDS. Clonotypic analysis of responses to B51-TI8 revealed a public clonotype using TRAV17/TRBV7-3 TCR genes in six out of seven HLA-B*51:01(+) patients. Structural analysis of a TRAV17/TRBV7-3 TCR in complex with HLA–B51-TI8, to our knowledge the first human TCR complexed with an 8-mer peptide, explained this bias, as the unique combination of residues encoded by these genes was central to the interaction. The relatively featureless peptide-MHC (pMHC) was mainly recognized by the TCR CDR1 and CDR2 loops in an MHC-centric manner. A highly conserved residue Arg(97) in the CDR3α loop played a major role in recognition of peptide and MHC to form a stabilizing ball-and-socket interaction with the MHC and peptide, contributing to the selection of the public TCR clonotype. Surface plasmon resonance equilibrium binding analysis showed the low affinity of this public TCR is in accordance with the only other 8-mer interaction studied to date (murine 2C TCR–H-2K(b)-dEV8). Like pMHC class II complexes, 8-mer peptides do not protrude out the MHC class I binding groove like those of longer peptides. The accumulated evidence suggests that weak affinity might be a common characteristic of TCR binding to featureless pMHC landscapes. AAI 2014-04-01 2014-03-05 /pmc/articles/PMC3962895/ /pubmed/24600035 http://dx.doi.org/10.4049/jimmunol.1302667 Text en Copyright © 2014 The Authors This is an open-access article distributed under the terms of the CC-BY 3.0 Unported license.
spellingShingle Molecular and Structural Immunology
Motozono, Chihiro
Kuse, Nozomi
Sun, Xiaoming
Rizkallah, Pierre J.
Fuller, Anna
Oka, Shinichi
Cole, David K.
Sewell, Andrew K.
Takiguchi, Masafumi
Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title_full Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title_fullStr Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title_full_unstemmed Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title_short Molecular Basis of a Dominant T Cell Response to an HIV Reverse Transcriptase 8-mer Epitope Presented by the Protective Allele HLA-B*51:01
title_sort molecular basis of a dominant t cell response to an hiv reverse transcriptase 8-mer epitope presented by the protective allele hla-b*51:01
topic Molecular and Structural Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3962895/
https://www.ncbi.nlm.nih.gov/pubmed/24600035
http://dx.doi.org/10.4049/jimmunol.1302667
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