Structural requirements for recognition of the HLA-Dw14 class II epitope: A key HLA determinant associated with rheumatoid arthritis

Hiraiwa, Akikazu; Yamanaka, Katsuo; Kwok, W W; Nepom, G T; Mickelson, E M; Masewicz, S; Hansen, J A; Radka, S F

doi:10.1073/pnas.87.20.8051

Title: Structural requirements for recognition of the HLA-Dw14 class II epitope: A key HLA determinant associated with rheumatoid arthritis

Journal Article · Mon Oct 01 00:00:00 EDT 1990 · Proceedings of the National Academy of Sciences of the United States of America; (USA)

DOI:https://doi.org/10.1073/pnas.87.20.8051· OSTI ID:5584554

Hiraiwa, Akikazu; Yamanaka, Katsuo; Kwok, W W; Nepom, G T ^[1]; Mickelson, E M; Masewicz, S; Hansen, J A ^[2]; Radka, S F ^[3]

Virginia Mason Research Center, Seattle, WA (USA)
Fred Hutchinson Cancer Research Center, Seattle, WA (USA)
Oncogen Corporation, Seattle, WA (USA)

Although HLA genes have been shown to be associated with certain diseases, the basis for this association is unknown. Recent studies, however, have documented patterns of nucleotide sequence variation among some HLA genes associated with a particular disease. For rheumatoid arthritis, HLA genes in most patients have a shared nucleotide sequence encoding a key structural element of an HLA class II polypeptide; this sequence element is critical for the interaction of the HLA molecule with antigenic peptides and with responding T cells, suggestive of a direct role for this sequence element in disease susceptibility. The authors describe the serological and cellular immunologic characteristics encoded by this rheumatoid arthritis-associated sequence element. Site-directed mutagenesis of the DRB1 gene was used to define amino acids critical for antibody and T-cell recognition of this structural element, focusing on residues that distinguish the rheumatoid arthritis-associated alleles Dw4 and Dw14 from a closely related allele, Dw10, not associated with disease. Both the gain and loss of rheumatoid arthritis-associated epitopes were highly dependent on three residues within a discrete domain of the HLA-DR molecule. Recognition was most strongly influenced by the following amino acids (in order): 70 > 71 > 67. Some alloreactive T-cell clones were also influenced by amino acid variation in portions of the DR molecule lying outside the shared sequence element.

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OSTI ID:: 5584554

Journal Information:: Proceedings of the National Academy of Sciences of the United States of America; (USA), Vol. 87:20; ISSN 0027-8424

Country of Publication:: United States

Language:: English

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59 BASIC BIOLOGICAL SCIENCES
HISTOCOMPATIBILITY COMPLEX
AMINO ACID SEQUENCE
RHEUMATIC DISEASES
ETIOLOGY
CODONS
DNA SEQUENCING
MONOCLONAL ANTIBODIES
MUTAGENESIS
PATIENTS
ANTIBODIES
ANTIGENS
DISEASES
MOLECULAR STRUCTURE
SKELETAL DISEASES
STRUCTURAL CHEMICAL ANALYSIS
550200* - Biochemistry

Title: Structural requirements for recognition of the HLA-Dw14 class II epitope: A key HLA determinant associated with rheumatoid arthritis

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