循环中的谷蛋白特异性而非巨细胞病毒特异性的CD39调节性T细胞具有寡克隆TCR库。

Circulating gluten-specific, but not CMV-specific, CD39 regulatory T cells have an oligoclonal TCR repertoire.

作者信息

Cook Laura, Munier C Mee Ling, Seddiki Nabila, Hardy Melinda Y, Anderson Robert P, Zaunders John, Tye-Din Jason A, Kelleher Anthony D, van Bockel David

机构信息

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Australia Sydney NSW Australia.

St Vincent's Centre for Applied Medical Research St Vincent's Hospital Sydney NSW Australia.

出版信息

Clin Transl Immunology. 2020 Jan 12;9(1):e1096. doi: 10.1002/cti2.1096. eCollection 2020.

DOI:10.1002/cti2.1096

PMID:31956412

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6955237/

Abstract

OBJECTIVES

Understanding the T cell receptor (TCR) repertoire of regulatory CD4 T-cell (Treg) populations is important for strategies aiming to re-establish tolerance in autoimmune diseases. We studied circulating deamidated gluten-epitope-specific CD39 Tregs in patients with coeliac disease following an oral gluten challenge, and we used cytomegalovirus (CMV)-specific CD39 Tregs from healthy controls as a comparator population.

METHODS

We used the OX40 assay to isolate antigen-specific Tregs by induced surface co-expression of CD25, OX40 and CD39. RACE PCR amplification and Sanger sequencing of the TCR β chain were used to analyse repertoire diversity.

RESULTS

We found that, following oral gluten challenge, circulating gluten-specific CD39 Tregs had an oligoclonal TCR repertoire that contained public clonotypes. Conversely, the TCR repertoire of CMV-epitope-specific CD39 Tregs from healthy controls was polyclonal.

DISCUSSION

These data indicate that a biased TCR repertoire is not inherent to CD39 Tregs, and, in this case, is apparently driven by the HLA-DQ2.5-restricted deamidated gluten peptide in coeliac disease patients.

CONCLUSION

This is the first assessment of the TCR repertoire within circulating human Tregs specific for foreign antigen. These data enhance our understanding of antigen-specific CD4 responses in the settings of chronic inflammation and infection and may help guide immunomonitoring strategies for CD4 T cell-based therapies, particularly for coeliac disease.

摘要

目的

了解调节性CD4 T细胞（Treg）群体的T细胞受体（TCR）库对于旨在重建自身免疫性疾病耐受性的策略至关重要。我们研究了乳糜泻患者口服麸质激发后循环中脱酰胺麸质表位特异性CD39 Treg，并用健康对照者的巨细胞病毒（CMV）特异性CD39 Treg作为对照群体。

方法

我们使用OX40检测法通过诱导CD25、OX40和CD39的表面共表达来分离抗原特异性Treg。采用RACE PCR扩增和TCR β链的桑格测序分析库多样性。

结果

我们发现，口服麸质激发后，循环中的麸质特异性CD39 Treg具有包含公共克隆型的寡克隆TCR库。相反，健康对照者的CMV表位特异性CD39 Treg的TCR库是多克隆的。

讨论

这些数据表明，偏向性的TCR库并非CD39 Treg所固有，在这种情况下，显然是由乳糜泻患者中HLA-DQ2.5限制的脱酰胺麸质肽驱动的。

结论

这是首次对循环中针对外来抗原的人类Treg内的TCR库进行评估。这些数据增进了我们对慢性炎症和感染情况下抗原特异性CD4反应的理解，并可能有助于指导基于CD4 T细胞疗法的免疫监测策略，特别是针对乳糜泻的策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cdaa/6955237/4e0c3047dbcb/CTI2-9-e1096-g001.jpg

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循环中的谷蛋白特异性而非巨细胞病毒特异性的CD39调节性T细胞具有寡克隆TCR库。

Circulating gluten-specific, but not CMV-specific, CD39 regulatory T cells have an oligoclonal TCR repertoire.

作者信息

Cook Laura, Munier C Mee Ling, Seddiki Nabila, Hardy Melinda Y, Anderson Robert P, Zaunders John, Tye-Din Jason A, Kelleher Anthony D, van Bockel David

机构信息

Immunovirology and Pathogenesis Program The Kirby Institute UNSW Australia Sydney NSW Australia.

St Vincent's Centre for Applied Medical Research St Vincent's Hospital Sydney NSW Australia.