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通过深度测序对克罗恩病患者炎症组织中T细胞受体库的特征分析

Characterization of T-cell Receptor Repertoire in Inflamed Tissues of Patients with Crohn's Disease Through Deep Sequencing.

作者信息

Chapman Christopher G, Yamaguchi Rui, Tamura Kenji, Weidner Jerome, Imoto Seiya, Kwon John, Fang Hua, Yew Poh Yin, Marino Susana R, Miyano Satoru, Nakamura Yusuke, Kiyotani Kazuma

机构信息

*Section of Gastroenterology, Department of Medicine, The University of Chicago, Chicago, Illinois; †Human Genome Center, Institute of Medical Science, The University of Tokyo, Tokyo, Japan; ‡Section of Hematology/Oncology, Department of Medicine, The University of Chicago, Chicago, Illinois; and §Department of Pathology, The University of Chicago, Chicago, Illinois.

出版信息

Inflamm Bowel Dis. 2016 Jun;22(6):1275-85. doi: 10.1097/MIB.0000000000000752.

Abstract

BACKGROUND

Intestinal tissues of patients with Crohn's disease (CD) contain expanded populations of T cells which are believed to mediate inflammation. We performed a detailed characterization of these T-cell repertoires.

METHODS

We obtained biopsies from the neoterminal ileum of 12 patients undergoing evaluation for postoperative recurrent CD and 4 individuals with normal terminal ileum and no history of inflammatory bowel disease (controls). Samples of diseased terminal ileum were obtained from 5 patients undergoing surgery for stricturing or penetrating CD. Total RNA was extracted from tissues and peripheral blood mononuclear cells, and cDNAs were generated. We used next-generation sequencing to characterize T-cell receptor (TCR)-α and TCR-β cDNAs in ileal mucosal tissue and matched peripheral blood mononuclear cells of 17 patients with CD to identify oligoclonal expansions of T-cell populations associated with CD.

RESULTS

TCR diversity in mucosal tissue was significantly lower than that of matched peripheral blood mononuclear cells, indicating expansion of certain T-cell populations in inflamed intestinal tissue. A single TCR-β clonotype, CASSWTNGEQYF (TRBV10-1-TRBJ2-7), was enriched at a frequency of 7.0% to 28.9% in the neoterminal ileum of 4 of 12 patients with recurrent CD. The abundance of this clonotype significantly correlated with the severity of disease recurrence, based on Rutgeerts score (P = 0.015).

CONCLUSIONS

Specific populations of T cells are expanded in the inflamed intestinal mucosa of patients with CD; their abundance correlates with severity of disease recurrence. Studies of these T cells could provide information about mechanisms of CD pathogenesis. Deep TCR sequencing is a powerful tool that rapidly provides in-depth, real-time assessment of the T-cell repertoire.

摘要

背景

克罗恩病(CD)患者的肠道组织中存在大量扩增的T细胞,据信这些T细胞介导炎症反应。我们对这些T细胞库进行了详细的特征分析。

方法

我们从12例接受术后复发性CD评估的患者的回肠末端新生物活检组织以及4例回肠末端正常且无炎症性肠病病史的个体(对照)获取样本。从5例因狭窄或穿透性CD接受手术的患者中获取病变回肠末端样本。从组织和外周血单个核细胞中提取总RNA,并生成cDNA。我们使用下一代测序技术对17例CD患者的回肠黏膜组织和匹配的外周血单个核细胞中的T细胞受体(TCR)-α和TCR-β cDNA进行特征分析,以鉴定与CD相关的T细胞群体的寡克隆扩增。

结果

黏膜组织中的TCR多样性显著低于匹配的外周血单个核细胞,表明炎症肠道组织中某些T细胞群体发生了扩增。一种单一的TCR-β克隆型CASSWTNGEQYF(TRBV10-1-TRBJ2-7)在12例复发性CD患者中的4例的回肠末端新生物中以7.0%至28.9%的频率富集。根据 Rutgeerts评分,这种克隆型的丰度与疾病复发的严重程度显著相关(P = 0.015)。

结论

CD患者炎症性肠黏膜中特定的T细胞群体发生了扩增;它们的丰度与疾病复发的严重程度相关。对这些T细胞的研究可为CD发病机制提供信息。深度TCR测序是一种强大的工具,可快速提供对T细胞库的深入实时评估。

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