INTERACTION OF THE PERTUSSIS TOXIN PEPTIDE CONTAINING RESIDUES-30-42 WITH DR1 AND THE T-CELL RECEPTORS OF 12 HUMAN T-CELL CLONES

被引:23
作者
DEMAGISTRIS, MT
DITOMMASO, A
DOMENIGHINI, M
CENSINI, S
TAGLIABUE, A
OKSENBERG, JR
STEINMAN, L
JUDD, AK
OSULLIVAN, D
RAPPUOLI, R
机构
[1] STANFORD UNIV,DEPT NEUROL & NEUROL SCI,STANFORD,CA 94305
[2] CYTEL,LA JOLLA,CA 92037
[3] SRI INT,BIOORGAN CHEM LAB,MENLO PK,CA 94025
关键词
T-CELL EPITOPE; PEPTIDE CONFORMATION; WHOOPING COUGH;
D O I
10.1073/pnas.89.7.2990
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
The interaction of the immunodominant pertussis toxin peptide containing residues 30-42 (p30-42) with soluble DR1 molecules and the T-cell receptor (TCR) of 12 DR1-restricted human T-cell clones has been analyzed. Peptide analogues of p30-42 containing single alanine substitutions were used in DR1-binding and T-cell proliferation assays to identify the major histocompatibility complex and TCR contact residues. Each T-cell clone was found to recognize p30-42 with a different fine specificity. However, a common core comprising amino acids 33-39 was found to be important for stimulation of all T-cell clones. Within this core two residues, Leu33 and Leu36, interact with the DR1 molecule, whereas Asp34, His35, Thr37, and Arg39 are important for TCR recognition in most of the clones. Computer modeling of the structure of p30-42 showed that an alpha-helical conformation is compatible with the experimental data. The analysis of TCR rearrangement revealed that the peptide was recognized by T-cell clones expressing different variable region alpha (V-alpha) and variable region beta (V-beta) chains, although a preferential use of V-alpha-8-V-beta-13 and V-alpha-11-V-beta-18 combinations was found in clones from the same donor. Understanding the details of the interaction of antigenic peptides with the major histocompatibility complex and TCR molecules should provide the theoretical basis to design T-cell epitopes and obtain more immunogenic vaccines.
引用
收藏
页码:2990 / 2994
页数:5
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