Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding

Michael Koch; Simon Camp; Trevor Collen; David Avila; Jan Salomonsen; Hans Joachim Wallny; Andrew van Hateren; Lawrence Hunt; Jansen P. Jacob; Fiona Johnston; Denise A A. Marston; Iain Shaw; P. Rod Dunbar; Vincenzo Cerundolo; E. Yvonne Jones; Jim Kaufman

doi:10.1016/j.immuni.2007.11.007

Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding

Michael Koch
, Simon Camp
, Trevor Collen
, David Avila
, Jan Salomonsen
, Hans Joachim Wallny
, Andrew van Hateren
, Lawrence Hunt
, Jansen P. Jacob
, Fiona Johnston
, Denise A A. Marston
, Iain Shaw
, P. Rod Dunbar
, Vincenzo Cerundolo
, E. Yvonne Jones
, Jim Kaufman

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

159 Citations (Scopus)

Abstract

Little is known about the structure of major histocompatibility complex (MHC) molecules outside of mammals. Only one class I molecule in the chicken MHC is highly expressed, leading to strong genetic associations with infectious pathogens. Here, we report two structures of the MHC class I molecule BF2^*2101 from the B21 haplotype, which is known to confer resistance to Marek's disease caused by an oncogenic herpesvirus. The binding groove has an unusually large central cavity, which confers substantial conformational flexibility to the crucial residue Arg9, allowing remodeling of key peptide-binding sites. The coupled variation of anchor residues from the peptide, utilizing a charge-transfer system unprecedented in MHC molecules, allows peptides with conspicuously different sequences to be bound. This promiscuous binding extends our understanding of ways in which MHC class I molecules can present peptides to the immune system and might explain the resistance of the B21 haplotype to Marek's disease.

Original language	English
Pages (from-to)	885-899
Number of pages	15
Journal	Immunity
Volume	27
Issue number	6
DOIs	https://doi.org/10.1016/j.immuni.2007.11.007
Publication status	Published - 21 Dec 2007
Externally published	Yes

Keywords

MOLIMMUNO

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10.1016/j.immuni.2007.11.007

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Koch, M., Camp, S., Collen, T., Avila, D., Salomonsen, J., Wallny, H. J., van Hateren, A., Hunt, L., Jacob, J. P., Johnston, F., Marston, DA. A., Shaw, I., Dunbar, P. R., Cerundolo, V., Jones, E. Y., & Kaufman, J. (2007). Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding. Immunity, 27(6), 885-899. https://doi.org/10.1016/j.immuni.2007.11.007

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title = "Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding",

abstract = "Little is known about the structure of major histocompatibility complex (MHC) molecules outside of mammals. Only one class I molecule in the chicken MHC is highly expressed, leading to strong genetic associations with infectious pathogens. Here, we report two structures of the MHC class I molecule BF2*2101 from the B21 haplotype, which is known to confer resistance to Marek's disease caused by an oncogenic herpesvirus. The binding groove has an unusually large central cavity, which confers substantial conformational flexibility to the crucial residue Arg9, allowing remodeling of key peptide-binding sites. The coupled variation of anchor residues from the peptide, utilizing a charge-transfer system unprecedented in MHC molecules, allows peptides with conspicuously different sequences to be bound. This promiscuous binding extends our understanding of ways in which MHC class I molecules can present peptides to the immune system and might explain the resistance of the B21 haplotype to Marek's disease.",

keywords = "MOLIMMUNO",

author = "Michael Koch and Simon Camp and Trevor Collen and David Avila and Jan Salomonsen and Wallny, \{Hans Joachim\} and \{van Hateren\}, Andrew and Lawrence Hunt and Jacob, \{Jansen P.\} and Fiona Johnston and Marston, \{Denise A A.\} and Iain Shaw and Dunbar, \{P. Rod\} and Vincenzo Cerundolo and Jones, \{E. Yvonne\} and Jim Kaufman",

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doi = "10.1016/j.immuni.2007.11.007",

language = "English",

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Koch, M, Camp, S, Collen, T, Avila, D, Salomonsen, J, Wallny, HJ, van Hateren, A, Hunt, L, Jacob, JP, Johnston, F, Marston, DAA, Shaw, I, Dunbar, PR, Cerundolo, V, Jones, EY & Kaufman, J 2007, 'Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding', Immunity, vol. 27, no. 6, pp. 885-899. https://doi.org/10.1016/j.immuni.2007.11.007

TY - JOUR

T1 - Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding

AU - Koch, Michael

AU - Camp, Simon

AU - Collen, Trevor

AU - Avila, David

AU - Salomonsen, Jan

AU - Wallny, Hans Joachim

AU - van Hateren, Andrew

AU - Hunt, Lawrence

AU - Jacob, Jansen P.

AU - Johnston, Fiona

AU - Marston, Denise A A.

AU - Shaw, Iain

AU - Dunbar, P. Rod

AU - Cerundolo, Vincenzo

AU - Jones, E. Yvonne

AU - Kaufman, Jim

PY - 2007/12/21

Y1 - 2007/12/21

N2 - Little is known about the structure of major histocompatibility complex (MHC) molecules outside of mammals. Only one class I molecule in the chicken MHC is highly expressed, leading to strong genetic associations with infectious pathogens. Here, we report two structures of the MHC class I molecule BF2*2101 from the B21 haplotype, which is known to confer resistance to Marek's disease caused by an oncogenic herpesvirus. The binding groove has an unusually large central cavity, which confers substantial conformational flexibility to the crucial residue Arg9, allowing remodeling of key peptide-binding sites. The coupled variation of anchor residues from the peptide, utilizing a charge-transfer system unprecedented in MHC molecules, allows peptides with conspicuously different sequences to be bound. This promiscuous binding extends our understanding of ways in which MHC class I molecules can present peptides to the immune system and might explain the resistance of the B21 haplotype to Marek's disease.

AB - Little is known about the structure of major histocompatibility complex (MHC) molecules outside of mammals. Only one class I molecule in the chicken MHC is highly expressed, leading to strong genetic associations with infectious pathogens. Here, we report two structures of the MHC class I molecule BF2*2101 from the B21 haplotype, which is known to confer resistance to Marek's disease caused by an oncogenic herpesvirus. The binding groove has an unusually large central cavity, which confers substantial conformational flexibility to the crucial residue Arg9, allowing remodeling of key peptide-binding sites. The coupled variation of anchor residues from the peptide, utilizing a charge-transfer system unprecedented in MHC molecules, allows peptides with conspicuously different sequences to be bound. This promiscuous binding extends our understanding of ways in which MHC class I molecules can present peptides to the immune system and might explain the resistance of the B21 haplotype to Marek's disease.

KW - MOLIMMUNO

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DO - 10.1016/j.immuni.2007.11.007

M3 - Article

SN - 1074-7613

VL - 27

SP - 885

EP - 899

JO - Immunity

JF - Immunity

IS - 6

ER -

Structures of an MHC Class I Molecule from B21 Chickens Illustrate Promiscuous Peptide Binding

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