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

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 NIB...

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Autores principales: Zhang, Ruijing, Xu, Keman, Shao, Ying, Sun, Yu, Saredy, Jason, Cutler, Elizabeth, Yao, Tian, Liu, Ming, Liu, Lu, Drummer IV, Charles, Lu, Yifan, Saaoud, Fatma, Ni, Dong, Wang, Jirong, Li, Yafeng, Li, Rongshan, Jiang, Xiaohua, Wang, Hong, Yang, Xiaofeng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7892453/
https://www.ncbi.nlm.nih.gov/pubmed/33613572
http://dx.doi.org/10.3389/fimmu.2020.632239
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author Zhang, Ruijing
Xu, Keman
Shao, Ying
Sun, Yu
Saredy, Jason
Cutler, Elizabeth
Yao, Tian
Liu, Ming
Liu, Lu
Drummer IV, Charles
Lu, Yifan
Saaoud, Fatma
Ni, Dong
Wang, Jirong
Li, Yafeng
Li, Rongshan
Jiang, Xiaohua
Wang, Hong
Yang, Xiaofeng
author_facet Zhang, Ruijing
Xu, Keman
Shao, Ying
Sun, Yu
Saredy, Jason
Cutler, Elizabeth
Yao, Tian
Liu, Ming
Liu, Lu
Drummer IV, Charles
Lu, Yifan
Saaoud, Fatma
Ni, Dong
Wang, Jirong
Li, Yafeng
Li, Rongshan
Jiang, Xiaohua
Wang, Hong
Yang, Xiaofeng
author_sort Zhang, Ruijing
collection PubMed
description 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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spelling pubmed-78924532021-02-20 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 Zhang, Ruijing Xu, Keman Shao, Ying Sun, Yu Saredy, Jason Cutler, Elizabeth Yao, Tian Liu, Ming Liu, Lu Drummer IV, Charles Lu, Yifan Saaoud, Fatma Ni, Dong Wang, Jirong Li, Yafeng Li, Rongshan Jiang, Xiaohua Wang, Hong Yang, Xiaofeng Front Immunol Immunology 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. Frontiers Media S.A. 2021-02-05 /pmc/articles/PMC7892453/ /pubmed/33613572 http://dx.doi.org/10.3389/fimmu.2020.632239 Text en Copyright © 2021 Zhang, Xu, Shao, Sun, Saredy, Cutler, Yao, Liu, Liu, Drummer IV, Lu, Saaoud, Ni, Wang, Li, Li, Jiang, Wang and Yang http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Zhang, Ruijing
Xu, Keman
Shao, Ying
Sun, Yu
Saredy, Jason
Cutler, Elizabeth
Yao, Tian
Liu, Ming
Liu, Lu
Drummer IV, Charles
Lu, Yifan
Saaoud, Fatma
Ni, Dong
Wang, Jirong
Li, Yafeng
Li, Rongshan
Jiang, Xiaohua
Wang, Hong
Yang, Xiaofeng
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
title 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
title_full 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
title_fullStr 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
title_full_unstemmed 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
title_short 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
title_sort 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
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7892453/
https://www.ncbi.nlm.nih.gov/pubmed/33613572
http://dx.doi.org/10.3389/fimmu.2020.632239
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