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Eur J Clin Invest. 1996 Dec;26(12):1092-102. doi: 10.1046/j.1365-2362.1996.440597.x.

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Dominant T-cell-receptor beta chain variable region V beta 14+ clones in juvenile rheumatoid arthritis.幼年类风湿关节炎中占主导地位的T细胞受体β链可变区Vβ14 +克隆
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Biased T cell receptor V gene usage in rheumatoid arthritis. Oligoclonal expansion of T cells expressing V alpha 2 genes in synovial fluid but not in peripheral blood.类风湿关节炎中T细胞受体V基因使用的偏向性。滑膜液中表达Vα2基因的T细胞呈寡克隆扩增,而外周血中则不然。
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Selection for T-cell receptor V beta-D beta-J beta gene rearrangements with specificity for a myelin basic protein peptide in brain lesions of multiple sclerosis.在多发性硬化症脑损伤中选择对髓鞘碱性蛋白肽具有特异性的T细胞受体Vβ-Dβ-Jβ基因重排。
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Prevention of type II collagen-induced arthritis by in vivo treatment with anti-L3T4.通过体内抗L3T4治疗预防II型胶原诱导的关节炎。
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Arthritis induced by a T-lymphocyte clone that responds to Mycobacterium tuberculosis and to cartilage proteoglycans.由对结核分枝杆菌和软骨蛋白聚糖有反应的T淋巴细胞克隆诱导的关节炎。
Proc Natl Acad Sci U S A. 1985 Aug;82(15):5117-20. doi: 10.1073/pnas.82.15.5117.
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Lymphoid V(D)J recombination: nucleotide insertion at signal joints as well as coding joints.淋巴细胞V(D)J重组:信号接头以及编码接头处的核苷酸插入。
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Selection of amino acid sequences in the beta chain of the T cell antigen receptor.T细胞抗原受体β链中氨基酸序列的选择
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Anti-idiotypic monoclonal antibody to a T-cell chronic lymphatic leukemia. Characterization of the antibody, in vitro effector functions and results of therapy.针对T细胞慢性淋巴细胞白血病的抗独特型单克隆抗体。抗体的特性、体外效应功能及治疗结果
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HLA genes associated with rheumatoid arthritis. Identification of susceptibility alleles using specific oligonucleotide probes.与类风湿性关节炎相关的HLA基因。使用特异性寡核苷酸探针鉴定易感等位基因。
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寡克隆类风湿性关节炎滑膜T细胞共有的CDR3序列基序。抗原驱动反应的证据。

CDR3 sequence motifs shared by oligoclonal rheumatoid arthritis synovial T cells. Evidence for an antigen-driven response.

作者信息

Li Y, Sun G R, Tumang J R, Crow M K, Friedman S M

机构信息

Department of Medicine, Hospital for Special Surgery, New York 10021.

出版信息

J Clin Invest. 1994 Dec;94(6):2525-31. doi: 10.1172/JCI117624.

DOI:10.1172/JCI117624
PMID:7989613
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC330088/
Abstract

T lymphocytes reactive with as yet undefined joint-localized foreign or autoantigens may be important in the pathogenesis of RA. Molecular studies demonstrating skewed T cell antigen receptor (TCR) variable gene usage and selective expansion of particular T cell clones within the synovial compartment support this view. Based on our recent study documenting selective expansion of V beta 17+ T cells in RA, we have pursued the identification of T cells relevant to the disease process, in an informative patient, by combining molecular analysis of freshly explanted RA synovial tissue V beta 17 TCR transcripts with in vitro expansion of V beta 17+ synovial tissue T cell clones. Peripheral blood V beta 17 cDNA transcripts proved heterogeneous. In contrast, two closely related sequences, not found in the peripheral blood, dominated synovial tissue V beta 17 transcripts, suggesting selective localization and oligoclonal expansion at the site of pathology. CD4+, V beta 17+ synovial tissue-derived T cell clones, isolated and grown in vitro, were found to express TCR beta chain transcripts homologous to the dominant V beta 17 synovial tissue sequences. One clone shares with a dominant synovial tissue sequence a conserved cluster of 4/5 amino acids (IGQ-N) in the highly diverse antigen binding CDR3 region, suggesting that the T cells from which these transcripts derive may recognize the same antigen. These findings have permitted a complete characterization of the alpha/beta TCR expressed by putatively pathogenic T cell clones in RA. Functional analysis suggests that the conserved CDR3 sequence may confer specificity for, or restriction by, the MHC class II antigen, DR4.

摘要

与尚未明确的关节局部外来或自身抗原发生反应的T淋巴细胞可能在类风湿性关节炎(RA)的发病机制中起重要作用。分子研究表明,滑膜腔内T细胞抗原受体(TCR)可变基因使用偏斜以及特定T细胞克隆的选择性扩增支持了这一观点。基于我们最近的一项研究记录了RA中Vβ17 + T细胞的选择性扩增,我们通过将新鲜切除的RA滑膜组织Vβ17 TCR转录本的分子分析与Vβ17 +滑膜组织T细胞克隆的体外扩增相结合,在一名信息丰富的患者中寻找与疾病过程相关的T细胞。外周血Vβ17 cDNA转录本被证明是异质性的。相比之下,在外周血中未发现的两个密切相关的序列主导了滑膜组织Vβ17转录本,表明在病理部位有选择性定位和寡克隆扩增。在体外分离并培养的CD4 +、Vβ17 +滑膜组织来源的T细胞克隆被发现表达与主导的Vβ17滑膜组织序列同源的TCRβ链转录本。一个克隆在高度多样化的抗原结合CDR3区域与一个主导的滑膜组织序列共享4/5个氨基酸的保守簇(IGQ-N),这表明这些转录本所源自的T细胞可能识别相同的抗原。这些发现使得能够完整地表征RA中假定的致病性T细胞克隆所表达的α/β TCR。功能分析表明,保守的CDR3序列可能赋予对II类主要组织相容性复合体抗原DR4的特异性或限制性。