The association of specific HLA-DQ alleles with autoimmunity is correlated with discrete polymorphisms in the HLA-DQ sequence that are localized within sites suitable for peptide recognition. The polymorphism at residue 57 of the DQB1 polypeptide is of particular interest since it may play a major structural role in the formation of a salt bridge structure at one end of the peptide-binding cleft of the DQ molecules. This polymorphism at residue 57 is a recurrent feature of HLA-DQ evolution, occurring in multiple distinct allelic families, which implies a functional selection for maintaining variation at this position in the class II molecule. We directly tested the amino acid polymorphism at this site as a determinant for peptide binding and for antigen-specific T cell stimulation. We found that a single Ala-->Asp amino acid 57 substitution in an HLA-DQ3.2 molecule regulated binding of an HSV-2 VP-16-derived peptide. A complementary single-residue substitution in the peptide abolished its binding to DQ3.2 and converted it to a peptide that can bind to DQ3.1 and DQ3.3 Asp-57-positive MHC molecules. These binding studies were paralleled by specific T cell recognition of the class II-peptide complex, in which the substituted peptide abolished T cell reactivity, which was directed to the DQ3.2-peptide complex, whereas the same T cell clone recognized the substituted peptide presented by DQ3.3, a class II restriction element differing from DQ3.2 only at residue 57. This structural and functional complementarity for residue 57 and a specific peptide residue identifies this interaction as a key controlling determinant of restricted recognition in HLA-DQ-specific immune response.
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1 March 1996
Article|
March 01 1996
HLA-DQB1 codon 57 is critical for peptide binding and recognition.
W W Kwok,
W W Kwok
Virginia Mason Research Center, Seattle, Washington 98101, USA.
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M E Domeier,
M E Domeier
Virginia Mason Research Center, Seattle, Washington 98101, USA.
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M L Johnson,
M L Johnson
Virginia Mason Research Center, Seattle, Washington 98101, USA.
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G T Nepom,
G T Nepom
Virginia Mason Research Center, Seattle, Washington 98101, USA.
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D M Koelle
D M Koelle
Virginia Mason Research Center, Seattle, Washington 98101, USA.
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W W Kwok
Virginia Mason Research Center, Seattle, Washington 98101, USA.
M E Domeier
Virginia Mason Research Center, Seattle, Washington 98101, USA.
M L Johnson
Virginia Mason Research Center, Seattle, Washington 98101, USA.
G T Nepom
Virginia Mason Research Center, Seattle, Washington 98101, USA.
D M Koelle
Virginia Mason Research Center, Seattle, Washington 98101, USA.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1996) 183 (3): 1253–1258.
Citation
W W Kwok, M E Domeier, M L Johnson, G T Nepom, D M Koelle; HLA-DQB1 codon 57 is critical for peptide binding and recognition.. J Exp Med 1 March 1996; 183 (3): 1253–1258. doi: https://doi.org/10.1084/jem.183.3.1253
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