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首页> 外文期刊>Genes and immunity. >Skewed T-cell receptor BV14 and BV16 expression and shared CDR3 sequence and common sequence motifs in synovial T cells of rheumatoid arthritis.
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Skewed T-cell receptor BV14 and BV16 expression and shared CDR3 sequence and common sequence motifs in synovial T cells of rheumatoid arthritis.

机译:类风湿关节炎滑膜T细胞中偏斜的T细胞受体BV14和BV16表达以及共享的CDR3序列和共有序列基序。

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摘要

T-lymphocytes play an important role in rheumatoid arthritis (RA). In this study, we evaluated the hypothesis that common T-cell receptor (TCR) structural features may exist among infiltrating T cells of different RA patients, if the TCR repertoire is shaped by interaction with common self or microbial antigens in the context of susceptible HLA genes in RA. Synovial lesion tissue (ST), synovial fluid (SF) and blood specimens from RA patients and controls were analyzed for TCR V gene repertoire by real-time PCR. There was highly skewed BV14 and BV16 usage in synovial T cells of RA as opposed to those of controls, which was accompanied with a trend for correlation between skewed BV16 and DRB1(*)0405. Immunoscope analysis of the V-D-J region of ST-derived T cells demonstrated oligoclonal and polyclonal expansion of BV14(+) and BV16(+) T cells. Detailed characterization using specific BV and BJ primers further revealed common clonotypes combining the same BV14/BV16, BJ and CDR3 length. DNA cloning and sequence analysis of the clonotypes confirmed identical CDR3 sequences and common CDR3 sequence motifs among different RA patients. The findings are important in the understanding of BV gene skewing and CDR3 structural characteristics among synovial infiltrating T cells of RA.
机译:T淋巴细胞在类风湿关节炎(RA)中起重要作用。在这项研究中,我们评估了以下假设:如果在易感性HLA的情况下通过与常见的自身或微生物抗原相互作用来塑造TCR组成,则不同RA患者的浸润T细胞之间可能存在共同的T细胞受体(TCR)结构特征RA中的基因。通过实时PCR分析RA患者和对照的滑膜病变组织(ST),滑液(SF)和血液标本的TCR V基因库。 RA的滑膜T细胞中BV14和BV16的使用偏高,与对照相比,这与偏斜的BV16和DRB1(*)0405之间的相关性趋势有关。对ST衍生T细胞的V-D-J区进行的免疫分析表明BV14(+)和BV16(+)T细胞具有寡克隆和多克隆扩增能力。使用特定的BV和BJ引物进行的详细表征进一步揭示了结合相同BV14 / BV16,BJ和CDR3长度的常见克隆型。 DNA克隆和克隆型的序列分析证实了不同RA患者之间相同的CDR3序列和常见的CDR3序列基序。这些发现对于理解RA滑膜浸润性T细胞之间的BV基因偏斜和CDR3结构特征非常重要。

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