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麻风分枝杆菌特异性T细胞表位、限制性HLA - DR2分子和两种特异性T细胞受体之间相互作用的分子图谱

Molecular mapping of interactions between a Mycobacterium leprae-specific T cell epitope, the restricting HLA-DR2 molecule, and two specific T cell receptors.

作者信息

Anderson D C, van Schooten W C, Janson A, Barry M E, de Vries R R

机构信息

Department of Pathobiology, University of Washington, Seattle 98119.

出版信息

J Immunol. 1990 Apr 1;144(7):2459-64.

PMID:1690768
Abstract

A systematic series of 89 single residue substitution analogs of the Mycobacterium leprae 65-kDa protein-derived peptide LQAAPALDKL were tested for stimulation of two HLA-DR2 restricted 65 kDa-reactive T cell clones from a tuberculoid leprosy patient. Some analogs with substitutions outside a "core" region showed enhanced stimulation of the T cell clones. This core region of seven or eight residues was essential for recognition, whereas substitution of amino acids outside this region did not affect T cell recognition although these residues could not be omitted. Thus these core residues interact directly with the presenting HLA-DR2 molecule and/or the TCR. Except for analogs of position 419 for clone 2B6, the majority of the nonstimulatory substitution analogs did not inhibit the presentation of LQAAPALDKL and thus probably failed to bind to the HLA-DR2 molecule. Unless all of the core residues are physically involved in binding to DR2, substitution at a position not directly involved in binding appears to have an influence on other residues that do bind to the DR2 molecule. Active peptide analogs with two or more internal prolines suggest that not all analogs need be helical for activity with clone 2F10.

摘要

对来自一名结核样麻风患者的89个麻风分枝杆菌65 kDa蛋白衍生肽LQAAPALDKL的单残基取代类似物进行了系统测试,以检测其对两个HLA - DR2限制的65 kDa反应性T细胞克隆的刺激作用。一些在“核心”区域之外有取代的类似物对T细胞克隆的刺激增强。这个由七八个残基组成的核心区域对于识别至关重要,而该区域之外的氨基酸取代并不影响T细胞识别,尽管这些残基不能省略。因此,这些核心残基直接与呈递的HLA - DR2分子和/或TCR相互作用。除了克隆2B6的419位类似物外,大多数无刺激作用的取代类似物并不抑制LQAAPALDKL的呈递,因此可能未能与HLA - DR2分子结合。除非所有核心残基都实际参与与DR2的结合,否则在不直接参与结合的位置进行取代似乎会对其他与DR2分子结合的残基产生影响。具有两个或更多内部脯氨酸的活性肽类似物表明,并非所有类似物都需要呈螺旋结构才能对克隆2F10产生活性。

相似文献

1
Molecular mapping of interactions between a Mycobacterium leprae-specific T cell epitope, the restricting HLA-DR2 molecule, and two specific T cell receptors.麻风分枝杆菌特异性T细胞表位、限制性HLA - DR2分子和两种特异性T细胞受体之间相互作用的分子图谱
J Immunol. 1990 Apr 1;144(7):2459-64.
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Functional analysis of DR17(DR3)-restricted mycobacterial T cell epitopes reveals DR17-binding motif and enables the design of allele-specific competitor peptides.DR17(DR3)限制性分枝杆菌T细胞表位的功能分析揭示了DR17结合基序,并有助于设计等位基因特异性竞争肽。
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Analysis of peptide residues interacting with MHC molecule or T cell receptor. Can a peptide bind in more than one way to the same MHC molecule?与MHC分子或T细胞受体相互作用的肽残基分析。一种肽能否以多种方式与同一MHC分子结合?
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A Mycobacterium leprae-specific human T cell epitope cross-reactive with an HLA-DR2 peptide.一种与HLA - DR2肽交叉反应的麻风分枝杆菌特异性人类T细胞表位。
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Mycobacterium leprae-specific T cells from a tuberculoid leprosy patient suppress HLA-DR3-restricted T cell responses to an immunodominant epitope on 65-kDa hsp of mycobacteria.一名结核样型麻风病患者的麻风分枝杆菌特异性T细胞可抑制HLA - DR3限制性T细胞对分枝杆菌65 kDa热休克蛋白上一个免疫显性表位的反应。
J Immunol. 1990 Dec 1;145(11):3898-904.

引用本文的文献

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J Virol. 1996 May;70(5):3108-17. doi: 10.1128/JVI.70.5.3108-3117.1996.
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Evolutionary conservation of major histocompatibility complex-DR/peptide/T cell interactions in primates.灵长类动物中主要组织相容性复合体-DR/肽/T细胞相互作用的进化保守性。
J Exp Med. 1993 Apr 1;177(4):979-87. doi: 10.1084/jem.177.4.979.
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Antigen-presenting capacity of rheumatoid synovial fibroblasts.
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Immunology. 1994 Jun;82(2):268-74.
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Interaction of the pertussis toxin peptide containing residues 30-42 with DR1 and the T-cell receptors of 12 human T-cell clones.含有30 - 42位残基的百日咳毒素肽与DR1及12个人类T细胞克隆的T细胞受体之间的相互作用。
Proc Natl Acad Sci U S A. 1992 Apr 1;89(7):2990-4. doi: 10.1073/pnas.89.7.2990.