Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease

Laura Cook; C. Mee Ling Munier; Nabila Seddiki; David van Bockel; Noé Ontiveros; Melinda Y. Hardy; Jana K. Gillies; Megan K. Levings; Hugh H. Reid; Jan Petersen; Jamie Rossjohn; Robert P. Anderson; John J. Zaunders; Jason A. Tye-Din; Anthony D. Kelleher

首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease

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Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease

机译：循环谷蛋白特异性Foxp3 + CD39 +调节T细胞对乳糜泻患者的抑制功能受损受损

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Background Celiac disease is a chronic immune-mediated inflammatory disorder of the gut triggered by dietary gluten. Although the effector T-cell response in patients with celiac disease has been well characterized, the role of regulatory T?Treg) cells in the loss of tolerance to gluten remains poorly understood. Objective We sought to define whether patients with celiac disease have a dysfunction or lack of gluten-specific forkhead box protein 3 (FOXP3) + Treg cells. Methods Treated patients with celiac disease underwent oral wheat challenge to stimulate recirculation of gluten-specific T cells. Peripheral blood was collected before and after challenge. To comprehensively measure the gluten-specific CD4 + T-cell response, we paired traditional IFN-?ELISpot with an assay to detect antigen-specific CD4 + T cells that does not rely on tetramers, antigen-stimulated cytokine production, or proliferation but rather on antigen-induced coexpression of CD25 and OX40 (CD134). Results Numbers of circulating gluten-specific Treg cells and effector T cells both increased significantly after oral wheat challenge, peaking at day 6. Surprisingly, we found that approximately 80% of the ex爒ivo circulating gluten-specific CD4 + T cells were FOXP3 + CD39 + Treg cells, which reside within the pool of memory CD4 + CD25 + CD127 low CD45RO + Treg cells. Although we observed normal suppressive function in peripheral polyclonal Treg cells from patients with celiac disease, after a short in爒itro expansion, the gluten-specific FOXP3 + CD39 + Treg cells exhibited significantly reduced suppressive function compared with polyclonal Treg cells. Conclusion This study provides the first estimation of FOXP3 + CD39 + Treg cell frequency within circulating gluten-specific CD4 + T cells after oral gluten challenge of patients with celiac disease. FOXP3 + CD39 + Treg cells comprised a major proportion of all circulating gluten-specific CD4 + T cells but had impaired suppressive function, indicating that Treg cell dysfunction might be a key contributor to disease pathogenesis.

机译：背景腹腔疾病是通过饮食面筋引发肠道的慢性免疫介导的炎症性疾病。尽管乳糜泻患者效应T细胞反应已被很好地表征，调节性T？Treg细胞）细胞的耐受损失的作用，面筋仍然知之甚少。目的我们试图确定乳糜泻患者是否有功能障碍或缺乏具体的麸质叉头框蛋白3（FOXP3）+ Treg细胞。方法治疗乳糜泻患者接受口服小麦的挑战，刺激特定的麸质的T细胞的再循环。外周血前与挑战后收集。全面测量面筋特异性CD4 + T细胞应答，我们配对传统IFN-γ酶联免疫斑点法用一种检测试验来检测不依赖于四聚体抗原特异性的CD4 + T细胞，抗原刺激细胞因子的产生，或增殖而是上CD25和OX40（CD134）的抗原诱导的共表达。结果循环面筋特异性调节性T细胞和效应T细胞的数量都口服后小麦的挑战显著上升，在第6天达到顶峰令人吃惊，我们发现前的大约80％爒IVO面筋特异性循环CD4 + T细胞FOXP3 + CD39 + Treg细胞，驻留存储器CD4 + CD25 + CD127低CD45RO + Treg细胞的池内。虽然我们在外围多克隆Treg细胞从乳糜泻患者观察到正常的抑制功能，在爒ITRO膨胀短后，麸质特异性的FOXP3 + CD39 + Treg细胞与多克隆Treg细胞相比表现出减少显著抑制功能。结论本研究后的乳糜泻患者口服面筋挑战提供FOXP3 + CD39 + Treg细胞频率的麸质特定循环CD4 + T细胞内的第一估计。 FOXP3 + CD39 + Treg细胞由循环面筋特定所有的CD4 + T细胞的主要比例，但已经受损的抑制功能，这表明Treg细胞功能障碍可能是一个关键因素，疾病的发病机制。

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来源
《The Journal of Allergy and Clinical Immunology 》 |2017年第6期| 共12页
作者
Laura Cook; C. Mee Ling Munier; Nabila Seddiki; David van Bockel; Noé Ontiveros; Melinda Y. Hardy; Jana K. Gillies; Megan K. Levings; Hugh H. Reid; Jan Petersen; Jamie Rossjohn; Robert P. Anderson; John J. Zaunders; Jason A. Tye-Din; Anthony D. Kelleher;
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作者单位

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

Immunology Division Walter and Eliza Hall Institute;

Immunology Division Walter and Eliza Hall Institute;

Department of Surgery University of British Columbia;

Department of Surgery University of British Columbia;

Infection and Immunity Program The Department of Biochemistry and Molecular Biology Biomedicine;

Infection and Immunity Program The Department of Biochemistry and Molecular Biology Biomedicine;

Infection and Immunity Program The Department of Biochemistry and Molecular Biology Biomedicine;

Immunology Division Walter and Eliza Hall Institute;

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

Immunology Division Walter and Eliza Hall Institute;

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Sydney;

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原文格式 PDF
正文语种 eng
中图分类医学免疫学 ;
关键词
Regulatory T cells; CD39; forkhead box protein 3; celiac disease; gluten; OX40;

机译：调节性T细胞;CD39;叉头箱蛋白3;乳糜泻;麸质;OX40;

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专利

1. Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease [J] . Laura Cook, C. Mee Ling Munier, Nabila Seddiki, The Journal of Allergy and Clinical Immunology . 2017 ,第6期

机译：循环谷蛋白特异性Foxp3 + CD39 +调节T细胞对乳糜泻患者的抑制功能受损受损
2. Circulating and intratumoral CD39(+)FoxP3(+) regulatory T cells associate with disease progression in HCC patients [J] . Fu Jun-Liang, Meng Fanping, Wang Fu-Sheng Hepatology: Official Journal of the American Association for the Study of Liver Diseases . 2016 ,第S1期

机译：循环和肿瘤内CD39（+）Foxp3（+）调节T细胞与HCC患者的疾病进展相关联
3. Decrease of CD4(+) CD25(+) CD127(low) FoxP3(+) regulatory T cells with impaired suppressive function in untreated ulcerative colitis patients [J] . Mohammadnia-Afrouzi Mousa, Hosseini Ahmad Zavaran, Khalili Ali, Autoimmunity . 2015 ,第8期

机译：未经治疗的溃疡性结肠炎患者抑制功能受损的CD4（+）CD25（+）CD127（低）FoxP3（+）调节性T细胞减少
4. Expression of CD4+CD25+ T regulatory cells and Foxp3 in peripheral blood of patients with Rheumatoid Arthritis Patient [C] . Kexin Sun, Yan Li, Suhong Guo, International Conference on Applied Science, Engineering and Technology . 2013

机译：类风湿性关节炎患者外周血CD4 + CD25 + T调节细胞和FOXP3的表达
5. Induction of Human CD39, Foxp3 and T Regulatory Cell Function by Bacteroides fragilis Polysaccharide A [D] . Telesford, Kiel Michael 2015

机译：脆弱拟杆菌（Bacteroides fragilis）多糖A诱导人CD39，Foxp3和T调节细胞功能
6. Decreased frequencies and impaired functions of the CD31+ subpopulation in Treg cells associated with decreased FoxP3 expression and enhanced Treg cell defects in patients with coronary heart disease [O] . L. Huang, Y. Zheng, X. Yuan, 2017

机译：冠心病患者Treg细胞中CD31 +亚群的频率降低和功能受损与FoxP3表达降低和Treg细胞缺陷增强相关
7. Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease [O] . Cook Laura, Munier C. Mee Ling, Seddiki Nabila, 2017

机译：麸质特异性循环蛋白FOXP3 + CD39 +调节性T细胞抑制了乳糜泻患者的抑制功能

Circulating gluten-specific FOXP3 + CD39 + regulatory T cells have impaired suppressive function in patients with celiac disease

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