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巨细胞动脉炎中克隆性扩增的T细胞受体序列的鉴定

Identification of clonally expanded T-cell receptor sequences in giant cell arteritis.

作者信息

Weber Anna, Zulcinski Michal, Haroon-Rashid Lubna, Kuszlewicz Beth, Driessen Alice, Newton Darren, Morgan Ann W, Rodríguez Martínez María

机构信息

International Buisness Machines Research Europe, Rüschlikon, 8803, Switzerland; Eidgenössische Technische Hochschule Zurich, Department of Biosystems Science and Engineering (D-BSSE), 4058, Basel, Switzerland.

School of Medicine, University of Leeds, Leeds, LS2 9JT, UK; NIHR Leeds Biomedical Research Centre, Leeds Teaching Hospitals NHS Trust, Leeds, UK.

出版信息

J Autoimmun. 2025 Feb;151:103372. doi: 10.1016/j.jaut.2025.103372. Epub 2025 Feb 3.

Abstract

BACKGROUND

Arterial wall inflammation in giant cell arteritis (GCA) is characterized by T-cell infiltration and granuloma formation. There have been limited studies investigating the diversity of the T-cell receptor (TCR) repertoire in GCA patients. Here we aim to identify disease-relevant TCRs.

METHODS

We sequenced the TCRβ repertoires in peripheral blood and biopsies from 72 GCA patients and compared them to repertoires of 60 age-matched controls. Applying K-nearest neighbours classification based on tcrdist3, an established TCR similarity measure, we identified GCA-associated TCRs across multiple model hyperparameters and experimental replicates.

RESULTS

We observed that species richness and Shannon diversity were significantly lower (P = 0.0003 and P = 0.004, respectively) in GCA peripheral blood TCR repertoires compared with age-matched controls. 1526 TCRs were identified that were consistently associated with GCA, 63 TCRs were also detected in TAB repertoires. Identical GCA-associated TCRs were observed in paired blood and tissue samples from 21/30 GCA cases. 57 % of GCA-associated TCRs were fitted into 10 clusters, which displayed distinct TCR sequences and TCR V and J segment usage. TRBV20-1∗01, TRBV4-3∗01, TRBV4-2∗01 and TRBV4-1∗01 segments were over-represented and occurred at least 10 % more often among GCA patients than age-matched controls. Only 27/1526 TCR sequences had matches reported in public databases, reducing the likelihood that these targeted common infectious agents.

CONCLUSIONS

Our data provide evidence of circulating T-cell clonal expansions in GCA patients. Certain TCR sequence patterns were over-represented in GCA subjects. As more TCR sequences directed at human antigens become available, further analysis may ultimately reveal whether these TCRs bind a common target antigen.

摘要

背景

巨细胞动脉炎(GCA)中的动脉壁炎症以T细胞浸润和肉芽肿形成为特征。对GCA患者T细胞受体(TCR)库多样性的研究有限。在此,我们旨在鉴定与疾病相关的TCR。

方法

我们对72例GCA患者外周血和活检组织中的TCRβ库进行测序,并将其与60例年龄匹配的对照者的TCRβ库进行比较。基于已建立的TCR相似性测量方法tcrdist3应用K近邻分类法,我们在多个模型超参数和实验重复中鉴定出与GCA相关的TCR。

结果

我们观察到,与年龄匹配的对照者相比,GCA外周血TCR库中的物种丰富度和香农多样性显著降低(分别为P = 0.0003和P = 0.004)。鉴定出1526个与GCA持续相关的TCR,在TAB库中也检测到63个TCR。在30例GCA患者中,有21例的配对血液和组织样本中观察到相同的与GCA相关的TCR。57%的与GCA相关的TCR被归入10个簇,这些簇显示出不同的TCR序列以及TCR V和J基因片段使用情况。TRBV20-1∗01、TRBV4-3∗01、TRBV4-2∗01和TRBV4-1∗01基因片段在GCA患者中过度表达,其出现频率比年龄匹配的对照者至少高10%。在公共数据库中仅报告了1526个TCR序列中的27个有匹配项,降低了这些TCR针对常见感染因子的可能性。

结论

我们的数据提供了GCA患者循环T细胞克隆扩增的证据。某些TCR序列模式在GCA受试者中过度表达。随着更多针对人类抗原的TCR序列可用,进一步分析最终可能揭示这些TCR是否结合共同的靶抗原。

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