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Biased T-cell receptor usage is associated with allelic variation in the MHC class II peptide binding groove
Authors:B Yassine-Diab  P Carmichael  Fatima-Ezzahra L'Faqihi  Giovanna Lombardi  Sarah Deacock  Claude de Préval  Hélène Coppin  R I Lechler
Institution:(1) U.395 INSERM, IFR 30 "INSERM-UPS-CNRS-CHU", CHU Purpan, Toulouse, France, FR;(2) ERS 1590 CNRS, IFR 30 "INSERM-UPS-CNRS-CHU", CHU Purpan, Toulouse, France, FR;(3) 4Department of Immunology, Royal Postgraduate Medical School, Du Cane Road, London W12 ONN, UK E-mail: rlechler@rpms.ac.uk, Tel. +44-181-3832088, Fax: +44-181-3832788, GB
Abstract: A comprehensive analysis was carried out of the tri-molecular complex of peptide, major histocompatibility class II molecule, and T-cell receptor (TcR) involved in the recognition of the promiscuous HA (306–318) peptide, restricted by one of two closely related HLA-DR alleles, HLA-DRB1*0101 and HLA-DRB1*0103. These two DR molecules differ by only three amino acids at positions 67, 70, and 71, in the third variable region of the DRB1 chain. None of the HA (306–318)-specific T-cell clones restricted by these two DR molecules tolerated amino acid substitution at the peptide-binding position 71, despite the fact that the substitution did not interfere with peptide binding. The majority of the DRB1*0103-restricted clones tolerated substitution of the amino acid at the TcR-contacting position 70, while the DRB1*0101-restricted T cells did not. Biased usage of TRVA and TRVB segments was observed for the DRB1*0103-restricted clones; in contrast, apparently random usage was seen in the DRB1*0101-restricted T cells. Finally, limiting dilution analysis revealed a lower frequency of T cells reactive with the HA peptide in a DRB1*0103 compared with a DRB1*0101 individual. Taken together these data suggest that biased TcR gene usage may reflect a relatively low precursor frequency of T cells, and the need for clonal expansion of a limited set of high avidity T cells. Received: 7 August 1998 / Revised: 19 November 1998
Keywords:  T-cell receptor  DR molecules  HA (306  318) peptide
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