FUNCTIONAL DEGENERACY OF RESIDUES IN A T-CELL PEPTIDE EPITOPE CONTRIBUTES TO ITS RECOGNITION BY DIFFERENT T-CELL HYBRIDOMAS

被引:12
作者
BOYER, M
NOVAK, Z
FRAGA, E
OIKAWA, K
KAY, CM
FOTEDAR, A
SINGH, B
机构
[1] UNIV ALBERTA,FAC MED,DEPT IMMUNOL,860 MED SCI BLDG,EDMONTON T6G 2H7,ALBERTA,CANADA
[2] UNIV ALBERTA,DEPT BIOCHEM,MRC CANADA,PROT STRUCT & FUNCT GRP,EDMONTON T6G 2H7,ALBERTA,CANADA
基金
英国医学研究理事会;
关键词
ANTIGEN RECOGNITION; PEPTIDE ANTIGENS; PEPTIDE VACCINES; AGRETOPES AND EPITOPES; MHC PEPTIDE BINDING GROOVE; ANTIGENIC COMPETITION; T-CELL RECEPTOR;
D O I
10.1093/intimm/2.12.1221
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Synthetic antigen Poly EYK(EYA)5 induces T cells of narrowly defined fine specificity as represented by the two I-A(d)-restricted T cell hybridomas, A.1.1. and B.1.1. Both these hybridomas recognize the minimum 15-amino-acid peptide sequence EYK(EYA)4. We have characterized the residues involved in the recognition of EYK(EYA)4 peptide by these hybridomas with synthetic peptides and discovered a distinct functional hierarchy for the residues in the sequence. Even with the repeating tripeptide (EYA)5, which is recognized by B.1.1 cells, the residues that are essential cluster near the middle of the sequence but not near the N- or C-terminal region. Different MHC binding and TCR contacting residues were found for each of the hybridomas. The results suggest that different T cells either recognize different parts of the peptide MHC complex or that the peptide binds to MHC in multiple conformations. This was supported by the fact that Poly EYK(EYA)5 is alpha-helical but the peptides used here showed only a slight propensity to adopt this structure and it did not correlate with their functional activity. We also found that (EYA)5 does not compete with EYK(EYA)4 in the stimulation of A.1.1 cells despite its obvious capacity to interact with I-A(d) when it stimulates B.1.1 cells. This may be because these peptides have a low affinity for la and therefore only appropriate TCR interactions would stabilize the antigen - la complex. In conclusion, antigen - MHC - TCR interaction appears to be a dynamic process which allows recognition of different residues of a T cell determinant by different T cells.
引用
收藏
页码:1221 / 1233
页数:13
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