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Genetic control of T cell receptor BJ gene expression in peripheral lymphocytes of normal and rheumatoid arthritis monozygotic twins.

机译:正常和类风湿关节炎单卵双胞胎的外周血T细胞受体BJ基因表达的遗传控制。

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摘要

The amino acids encoded at the junctions of T cell receptor (TCR) V and J genes directly interact with MHC bound peptides. However, the regulation of the human TCRBJ gene repertoire has been difficult to analyze, because of the potentially complex number of BJ gene rearrangements. To overcome this problem, we developed a PCR-ELISA method to study BJ gene expression, and compared peripheral T lymphocytes from 12 pairs of monozygotic twins, including 6 rheumatoid arthritis (RA) discordant pairs, and 5 normals. Analyses of the TCRBV5, 13 and 17 gene families, which have been reported to be increased in RA patients, showed: (a) the three TCRBV transcripts have common features of BJ gene usage; (b) TCR transcripts from each TCRBV family display a distinctive BJ gene profile, which is displayed better by CD4+ than CD8+ lymphocytes; (c) the BJ gene repertoires of monozygotic twins are more similar than those of unrelated individuals; and (d) the inflammation of RA does not induce specific changes in the genetically determined pattern of BJ expression. These results indicate that the frequency of expression particular TCRBV-TCRBJ recombinants in human lymphocytes is controlled genetically, and is maintained despite the presence of a chronic inflammatory disease.
机译:T细胞受体(TCR)V和J基因交界处编码的氨基酸直接与MHC结合的肽相互作用。但是,由于BJ基因重排的潜在复杂性,很难分析人TCRBJ基因库的调控。为了克服这个问题,我们开发了一种PCR-ELISA方法来研究BJ基因表达,并比较了12对单卵双胞胎的外周T淋巴细胞,包括6对类风湿关节炎(RA)不和谐对和5对正常人。对据报道在RA患者中增加的TCRBV5、13和17基因家族的分析显示:(a)三种TCRBV转录本具有BJ基因使用的共同特征; (b)来自每个TCRBV家族的TCR转录本显示出独特的BJ基因谱,其中CD4 +的表现优于CD8 +的淋巴细胞; (c)单卵双胞胎的BJ基因组成比无亲属的个体更相似; (d)RA的炎症不会引起BJ表达的遗传学确定模式的特异性变化。这些结果表明,特定TCRBV-TCRBJ重组体在人淋巴细胞中表达的频率是遗传控制的,尽管存在慢性炎性疾病也可以保持。

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