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类风湿关节炎期间滑膜组织中优势T细胞克隆的持续性。

Persistence of dominant T cell clones in synovial tissues during rheumatoid arthritis.

作者信息

Alam A, Lambert N, Lulé J, Coppin H, Mazières B, de Préval C, Cantagrel A

机构信息

National Institute for Health and Medical Research (INSERM) Unit 395, Purpan Hospital, Toulouse, France.

出版信息

J Immunol. 1996 May 1;156(9):3480-5.

PMID:8617976
Abstract

In a previous study, we showed that the T cell repertoire is biased in the synovial membrane (SM) compared with peripheral blood during rheumatoid arthritis (RA). The same bias was observed in different joints from the same patient and seems to be the same over time. To discover whether this bias was due to expansion of a clonal subset resulting from activation by conventional Ag(s) or to polygonal stimulation by superantigen(s), we sequenced more than 650 TCRBV-D-J junctional regions from freshly isolated SM and peripheral blood of two DR4-RA patients. From each patient, two SM were obtained on the same day, and a third was obtained later. Several dominant clones were found in SM but not in peripheral blood. Some of them were found only at the first time point in anatomically different SM, the majority persisted over time, and others were detected only at the second time point. Analysis of the complementarity-determining region 3 (CDR3) showed a bias in TCRBD and amino acid usage. Valine, encoded by randomly inserted N nucleotides, was used by 45% of dominant clones compared with 18% in the control population (p less than 0.001). In addition, GXXG and TSG motifs were frequently observed in the CDR3 of these dominant clones. These data indicate a dynamic TCR selection process during the perpetuation phase of RA. The dynamic changes of dominant clones also suggest a determinant spreading mechanism during RA.

摘要

在之前的一项研究中,我们发现,与类风湿关节炎(RA)患者外周血相比,其滑膜(SM)中的T细胞库存在偏向性。在同一患者的不同关节中也观察到了同样的偏向性,并且似乎随时间保持一致。为了探究这种偏向性是由于传统抗原激活导致的克隆亚群扩增,还是由于超抗原的多克隆刺激,我们对两名DR4-RA患者新鲜分离的滑膜和外周血中650多个TCRBV-D-J连接区进行了测序。从每位患者同一天获取两个滑膜样本,之后再获取第三个样本。在滑膜中发现了几个优势克隆,但在外周血中未发现。其中一些仅在解剖学上不同的滑膜的第一个时间点被发现,大多数随时间持续存在,其他的则仅在第二个时间点被检测到。互补决定区3(CDR3)分析显示TCRBD和氨基酸使用存在偏向性。由随机插入的N核苷酸编码的缬氨酸,在45%的优势克隆中被使用,而在对照群体中这一比例为18%(p<0.001)。此外,在这些优势克隆的CDR3中经常观察到GXXG和TSG基序。这些数据表明在RA持续阶段存在动态的TCR选择过程。优势克隆的动态变化也提示了RA期间的决定簇扩展机制。

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