Preferential peptide specificity and HLA restriction of myelin basic protein-specific T cell clones derived from MS patients

A panel of 17 myelin basic protein (MBP)-specific T lymphocyte clones were generated from four multiple sclerosis (MS) patients. All T cell clones expressed CD4 phenotype and 14 clones exhibited substantial cytotoxic activity on MBP-coated target cells. T cell recognition sites of the clones on huma...

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Veröffentlicht in:Cellular immunology 1990-08, Vol.129 (1), p.189-198
Hauptverfasser: Jingwu, Zhang, Chou, Chi-Hsin J., Hashim, George, Medaer, Robert, Raus, Jef C.M.
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container_end_page 198
container_issue 1
container_start_page 189
container_title Cellular immunology
container_volume 129
creator Jingwu, Zhang
Chou, Chi-Hsin J.
Hashim, George
Medaer, Robert
Raus, Jef C.M.
description A panel of 17 myelin basic protein (MBP)-specific T lymphocyte clones were generated from four multiple sclerosis (MS) patients. All T cell clones expressed CD4 phenotype and 14 clones exhibited substantial cytotoxic activity on MBP-coated target cells. T cell recognition sites of the clones on human MBP were identified by using MBP fragments and synthetic peptides. Despite the fact that at least three epitopes were defined, these T cell clones displayed a striking bias to the C-terminal peptide 149–171 independent of differences in HLA-DR and DQ expression. In addition, the T cell responses of the clones appeared to be restricted by HLA-DR molecules irrespective of peptide specificities. The present study suggests an immunodominant property of the C-terminal peptide for HLA-DR-restricted T cell responses to MBP. However, its association with encephalitogenicity in humans and its potential pathologic importance in MS await further clarification.
doi_str_mv 10.1016/0008-8749(90)90197-Y
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All T cell clones expressed CD4 phenotype and 14 clones exhibited substantial cytotoxic activity on MBP-coated target cells. T cell recognition sites of the clones on human MBP were identified by using MBP fragments and synthetic peptides. Despite the fact that at least three epitopes were defined, these T cell clones displayed a striking bias to the C-terminal peptide 149–171 independent of differences in HLA-DR and DQ expression. In addition, the T cell responses of the clones appeared to be restricted by HLA-DR molecules irrespective of peptide specificities. The present study suggests an immunodominant property of the C-terminal peptide for HLA-DR-restricted T cell responses to MBP. 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Guillain barré syndrome and other inflammatory polyneuropathies. 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subjects Amino Acid Sequence
Biological and medical sciences
CD4-Positive T-Lymphocytes - immunology
Clone Cells
Cytotoxicity, Immunologic
Epitopes - immunology
HLA-D Antigens - immunology
Humans
Medical sciences
Molecular Sequence Data
Multiple Sclerosis - immunology
Multiple sclerosis and variants. Guillain barré syndrome and other inflammatory polyneuropathies. Leukoencephalitis
Myelin Basic Protein - immunology
Neurology
Peptide Fragments - immunology
Phenotype
T-Lymphocytes - immunology
title Preferential peptide specificity and HLA restriction of myelin basic protein-specific T cell clones derived from MS patients
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