与干细胞共享的组织Treg分泌组和转录因子有助于Treg生态位维持80%先天免疫途径的Treg性，以及免疫抑制和组织修复功能。

IF 5.7 2区医学 Q1 IMMUNOLOGY

Frontiers in Immunology Pub Date : 2020-01-01 DOI:10.3389/fimmu.2020.632239

Ruijing Zhang, Keman Xu, Ying Shao, Yu Sun, Jason Saredy, Elizabeth Cutler, Tian Yao, Ming Liu, Lu Liu, Charles Drummer Iv, Yifan Lu, Fatma Saaoud, Dong Ni, Jirong Wang, Yafeng Li, Rongshan Li, Xiaohua Jiang, Hong Wang, Xiaofeng Yang

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引用次数: 25

摘要

我们利用功能组学角度，检测了来自脾脏(s-Treg)、淋巴结(LN-Treg)、肠道(int-Treg)和内脏脂肪组织(fat -Treg)的CD4+Foxp3+调节性T细胞(Treg)的转录组异质性，得到了重要发现:1)鉴定出5个新的共享Treg基因，包括NIBAN、TNFRSF1b、DUSP4、VAV2和KLRG1，并鉴定出68个新的特征。在4种组织Treg共有的27条信号通路中，先天免疫通路22条(81.5%);2) s-Treg、LN-Treg、int-Treg和VAT-Treg分别有0、49、45和116条上调通路;3) 373个CD标记物中分别有12个、7个和15个被鉴定为特异于LN-Treg、int-Treg和VAT-Treg，它们可能启动先天免疫信号;4)在1176个细胞因子中，4个Treg分别有7、49、44和79个细胞因子增加，表明Treg比IL-10、TGF-β和IL-35具有更多的分泌蛋白/细胞因子;5)通过分析1706个分泌基因，发现LN-Treg、int-Treg和VAT-Treg比s-Treg多出13个额外的分泌功能;6) 1496个增加的转录因子(TFs)中，分别有2、20、25和43个被鉴定为4个Treg;7) LN-Treg和int-Treg增加了焦亡调节因子，而VAT-Treg增加了凋亡调节因子;8) 661个kinome中分别鉴定出1、15、19和31个与s-Treg、LN-Treg、int-Treg和VAT-Treg相关的增加激酶;9)与s-Treg、LN-Treg、int-Treg和VAT-Treg相比，激活的簇(1-3簇)标志物增加;降低静息聚类(聚类4-6)标志物;10) Treg通过与干细胞共享分泌组和tf AHR、ETV5、EGR1和KLF4来促进组织修复，这部分促进了Treg各组基因的上调。这些结果表明，干细胞共享主基因使组织Treg成为第一个使用Treg生态位维持其Treg性的T细胞类型，具有80%的先天免疫途径，并具有免疫抑制、组织修复和维持体内平衡的三重功能。我们的研究结果为先天免疫途径在Treg异质性中的作用提供了新的见解，并为免疫抑制、组织修复、心血管疾病、慢性肾脏疾病、自身免疫性疾病、移植和癌症提供了新的治疗靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Tissue Treg Secretomes and Transcription Factors Shared With Stem Cells Contribute to a Treg Niche to Maintain Treg-Ness With 80% Innate Immune Pathways, and Functions of Immunosuppression and Tissue Repair.

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We used functional -omics angles and examined transcriptomic heterogeneity in CD4⁺Foxp3⁺ regulatory T cells (Treg) from spleen (s-Treg), lymph nodes (LN-Treg), intestine (int-Treg), and visceral adipose tissue (VAT-Treg), and made significant findings: 1) Five new shared Treg genes including NIBAN, TNFRSF1b, DUSP4,VAV2, and KLRG1, and 68 new signatures are identified. Among 27 signaling pathways shared in four tissue Treg, 22 pathways are innate immune pathways (81.5%); 2) s-Treg, LN-Treg, int-Treg, and VAT-Treg have zero, 49, 45, and 116 upregulated pathways, respectively; 3) 12, 7, and 15 out of 373 CD markers are identified as specific for LN-Treg, int-Treg, and VAT-Treg, respectively, which may initiate innate immune signaling; 4) 7, 49, 44, and 79 increased cytokines out of 1176 cytokines are identified for four Treg, respectively, suggesting that Treg have much more secretory proteins/cytokines than IL-10, TGF-β, and IL-35; 5) LN-Treg, int-Treg, and VAT-Treg have 13 additional secretory functions more than s-Treg, found by analyzing 1,706 secretomic genes; 6) 2, 20, 25, and 43 increased transcription factors (TFs) out of 1,496 TFs are identified four Treg, respectively; 7) LN-Treg and int-Treg have increased pyroptosis regulators but VAT-Treg have increased apoptosis regulators; 8) 1, 15, 19, and 31 increased kinases out of 661 kinome are identified for s-Treg, LN-Treg, int-Treg, and VAT-Treg, respectively; 9) comparing with that of s-Treg, LN-Treg, int-Treg, and VAT-Treg increase activated cluster (clusters 1-3) markers; and decrease resting cluster (clusters 4-6) markers; and 10) Treg promote tissue repair by sharing secretomes and TFs AHR, ETV5, EGR1, and KLF4 with stem cells, which partially promote upregulation of all the groups of Treg genes. These results suggest that stem cell-shared master genes make tissue Treg as the first T cell type using a Treg niche to maintain their Treg-ness with 80% innate immune pathways, and triple functions of immunosuppression, tissue repair, and homeostasis maintenance. Our results have provided novel insights on the roles of innate immune pathways on Treg heterogeneity and new therapeutic targets for immunosuppression, tissue repair, cardiovascular diseases, chronic kidney disease, autoimmune diseases, transplantation, and cancers.

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来源期刊

Frontiers in Immunology IMMUNOLOGY-

CiteScore

9.80

自引率

11.00%

发文量

7153

审稿时长

14 weeks

期刊介绍： Frontiers in Immunology is a leading journal in its field, publishing rigorously peer-reviewed research across basic, translational and clinical immunology. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. Frontiers in Immunology is the official Journal of the International Union of Immunological Societies (IUIS). Encompassing the entire field of Immunology, this journal welcomes papers that investigate basic mechanisms of immune system development and function, with a particular emphasis given to the description of the clinical and immunological phenotype of human immune disorders, and on the definition of their molecular basis.