High resolution structures of highly bulged viral epitopes bound to major histocompatibility complex class I. Implications for T-cell receptor engagement and T-cell immunodominance

High resolution structures of highly bulged viral epitopes bound to major histocompatibility complex class I. Implications for T-cell receptor engagement and T-cell immunodominance

Although HLA class I alleles can bind epitopes up to 14 amino acids in length, little is known about the immunogenicity or the responding T-cell repertoire against such determinants. Here, we describe an HLA-B*3508-restricted cytotoxic T lymphocyte response to a 13-mer viral epitope (LPEPLPQGQLTAY)....

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Veröffentlicht in:The Journal of biological chemistry 2005-06, Vol.280 (25), p.23900-23909
Hauptverfasser: Tynan, Fleur E, Borg, Natalie A, Miles, John J, Beddoe, Travis, El-Hassen, Diah, Silins, Sharon L, van Zuylen, Wendy J M, Purcell, Anthony W, Kjer-Nielsen, Lars, McCluskey, James, Burrows, Scott R, Rossjohn, Jamie
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Sprache:eng
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Amino Acid Sequence
Base Sequence
Cell Line
Flow Cytometry
Histocompatibility Antigens Class I - metabolism
Humans
Immunodominant Epitopes - chemistry
Immunodominant Epitopes - metabolism
Models, Molecular
Molecular Sequence Data
Molecular Structure
Receptors, Antigen, T-Cell - metabolism
T-Lymphocytes, Cytotoxic - immunology
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container_end_page 23909
container_issue 25
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container_title The Journal of biological chemistry
container_volume 280
creator Tynan, Fleur E
Borg, Natalie A
Miles, John J
Beddoe, Travis
El-Hassen, Diah
Silins, Sharon L
van Zuylen, Wendy J M
Purcell, Anthony W
Kjer-Nielsen, Lars
McCluskey, James
Burrows, Scott R
Rossjohn, Jamie
description Although HLA class I alleles can bind epitopes up to 14 amino acids in length, little is known about the immunogenicity or the responding T-cell repertoire against such determinants. Here, we describe an HLA-B*3508-restricted cytotoxic T lymphocyte response to a 13-mer viral epitope (LPEPLPQGQLTAY). The rigid, centrally bulged epitope generated a biased T-cell response. Only the N-terminal face of the peptide bulge was critical for recognition by the dominant clonotype SB27. The SB27 public T-cell receptor (TcR) associated slowly onto the complex between the bulged peptide and the major histocompatibility complex, suggesting significant remodeling upon engagement. The broad antigen-binding cleft of HLA-B*3508 represents a critical feature for engagement of the public TcR, as the narrower binding cleft of HLA-B*3501(LPEPLPQGQLTAY), which differs from HLA-B*3508 by a single amino acid polymorphism (Arg156 --> Leu), interacted poorly with the dominant TcR. Biased TcR usage in this cytotoxic T lymphocyte response appears to reflect a dominant role of the prominent peptide x major histocompatibility complex class I surface.
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subjects Amino Acid Sequence
Base Sequence
Cell Line
Flow Cytometry
Histocompatibility Antigens Class I - metabolism
Humans
Immunodominant Epitopes - chemistry
Immunodominant Epitopes - metabolism
Models, Molecular
Molecular Sequence Data
Molecular Structure
Receptors, Antigen, T-Cell - metabolism
T-Lymphocytes, Cytotoxic - immunology
title High resolution structures of highly bulged viral epitopes bound to major histocompatibility complex class I. Implications for T-cell receptor engagement and T-cell immunodominance
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