Bound water structure and polymorphic amino acids act together to allow the binding of different peptides to MHC class I HLA-B53

被引：152

作者：

Smith, KJ

Reid, SW

Harlos, K

McMichael, AJ

Stuart, DI

Bell, JI

Jones, EY

机构：

[1] JOHN RADCLIFFE HOSP, INST MOLEC MED, NUFFIELD DEPT CLIN MED, MOLEC IMMUNOL GRP, OXFORD OX3 9DU, ENGLAND

[2] UNIV OXFORD, MOLEC BIOPHYS LAB, OXFORD OX1 3QU, ENGLAND

[3] UNIV OXFORD, OXFORD CTR MOLEC SCI, DEPT BIOCHEM, OXFORD OX1 3QU, ENGLAND

来源：

IMMUNITY | 1996年 / 4卷 / 03期

基金：

英国惠康基金;

关键词：

D O I：

10.1016/S1074-7613(00)80430-6

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

The structure of the human MHC class I molecule HLA-B53 complexed to two nonameric peptide epitopes (from the malaria parasite P. falciparum and the HIV2 gag protein) has been determined by X-ray crystallography at 2.3 Angstrom resolution. The structures reveal the architecture of a Pro-specific B pocket common to many HLA-B alleles. Relative to other alleles, the B53 peptide-binding groove is widened by a significant (up to 1.25 Angstrom) shift in the position of the al helix. Within this groove, bound water molecules, acting in concert with the side chains of polymorphic residues, provide the functional malleability of the MHC, which enables the high affinity/low specificity binding of multiple peptide epitopes.

引用

页码：215 / 228

页数：14

共 45 条

[1] SEQUENCE-ANALYSIS OF HLA-BW53, A COMMON WEST AFRICAN ALLELE, SUGGESTS AN ORIGIN BY GENE CONVERSION OF HLA-B35
ALLSOPP, CEM
HILL, AVS
KWIATKOWSKI, D
HUGHES, A
BUNCE, M
TAYLOR, CJ
PAZMANY, L
BREWSTER, D
MCMICHAEL, AJ
GREENWOOD, BM
[J]. HUMAN IMMUNOLOGY, 1991, 30 (02) : 105 - 109
[2] THE CCP4 SUITE - PROGRAMS FOR PROTEIN CRYSTALLOGRAPHY
BAILEY, S
[J]. ACTA CRYSTALLOGRAPHICA SECTION D-BIOLOGICAL CRYSTALLOGRAPHY, 1994, 50 : 760 - 763
[3] OVERLAP IN THE REPERTOIRES OF PEPTIDES BOUND IN-VIVO BY A GROUP OF RELATED CLASS-I HLA-B ALLOTYPES
BARBER, LD
GILLECECASTRO, B
PERCIVAL, L
LI, XB
CLAYBERGER, C
PARHAM, P
[J]. CURRENT BIOLOGY, 1995, 5 (02) : 179 - 190
[4] STRUCTURE OF THE HUMAN CLASS-I HISTOCOMPATIBILITY ANTIGEN, HLA-A2
BJORKMAN, PJ
SAPER, MA
SAMRAOUI, B
BENNETT, WS
STROMINGER, JL
WILEY, DC
[J]. NATURE, 1987, 329 (6139) : 506 - 512
[5] BRUGER AT, 1990, ACTA CRYSTALLOGR A, V46, P585
[6] BRUNGER AT, 1992, XPLOR VERSION 3 1 SY
[7] 3-DIMENSIONAL STRUCTURE OF A PEPTIDE EXTENDING FROM ONE END OF A CLASS-I MHC BINDING-SITE
COLLINS, EJ
GARBOCZI, DN
WILEY, DC
[J]. NATURE, 1994, 371 (6498) : 626 - 629
[8] RECOGNITION BY CD8 ON CYTOTOXIC LYMPHOCYTES-T IS ABLATED BY SEVERAL SUBSTITUTIONS IN THE CLASS-I ALPHA-3 DOMAIN - CD8 AND THE T-CELL RECEPTOR RECOGNIZE THE SAME CLASS-I MOLECULE
CONNOLLY, JM
HANSEN, TH
INGOLD, AL
POTTER, TA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (06) : 2137 - 2141
[9] ENDOGENOUS PEPTIDES OF A SOLUBLE MAJOR HISTOCOMPATIBILITY COMPLEX CLASS-I MOLECULE, H-2L(D)(S) - SEQUENCE MOTIF, QUANTITATIVE BINDING, AND MOLECULAR MODELING OF THE COMPLEX
CORR, M
BOYD, LF
FRANKEL, SR
KOZLOWSKI, S
PADLAN, EA
MARGULIES, DH
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1992, 176 (06) : 1681 - 1692
[10] PEPTIDE SELECTION BY CLASS-I MOLECULES OF THE MAJOR HISTOCOMPATIBILITY COMPLEX
ELLIOTT, T
SMITH, M
DRISCOLL, P
MCMICHAEL, A
[J]. CURRENT BIOLOGY, 1993, 3 (12) : 854 - 866

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