Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease

There has been much interest in the ability of regulatory T cells (Treg) to switch function in vivo, either as a result of genetic risk of disease or in response to environmental and metabolic cues. The relationship between levels of FOXP3 and functional fitness plays a significant part in this plas...

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Autores principales: Brown, Cheryl Y., Sadlon, Timothy, Hope, Christopher M., Wong, Ying Y., Wong, Soon, Liu, Ning, Withers, Holly, Brown, Katherine, Bandara, Veronika, Gundsambuu, Batjargal, Pederson, Stephen, Breen, James, Robertson, Sarah Anne, Forrest, Alistair, Beyer, Marc, Barry, Simon Charles
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7533603/
https://www.ncbi.nlm.nih.gov/pubmed/33072063
http://dx.doi.org/10.3389/fimmu.2020.01269
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author Brown, Cheryl Y.
Sadlon, Timothy
Hope, Christopher M.
Wong, Ying Y.
Wong, Soon
Liu, Ning
Withers, Holly
Brown, Katherine
Bandara, Veronika
Gundsambuu, Batjargal
Pederson, Stephen
Breen, James
Robertson, Sarah Anne
Forrest, Alistair
Beyer, Marc
Barry, Simon Charles
author_facet Brown, Cheryl Y.
Sadlon, Timothy
Hope, Christopher M.
Wong, Ying Y.
Wong, Soon
Liu, Ning
Withers, Holly
Brown, Katherine
Bandara, Veronika
Gundsambuu, Batjargal
Pederson, Stephen
Breen, James
Robertson, Sarah Anne
Forrest, Alistair
Beyer, Marc
Barry, Simon Charles
author_sort Brown, Cheryl Y.
collection PubMed
description There has been much interest in the ability of regulatory T cells (Treg) to switch function in vivo, either as a result of genetic risk of disease or in response to environmental and metabolic cues. The relationship between levels of FOXP3 and functional fitness plays a significant part in this plasticity. There is an emerging role for Treg in tissue repair that may be less dependent on FOXP3, and the molecular mechanisms underpinning this are not fully understood. As a result of detailed, high-resolution functional genomics, the gene regulatory networks and key functional mediators of Treg phenotype downstream of FOXP3 have been mapped, enabling a mechanistic insight into Treg function. This transcription factor-driven programming of T-cell function to generate Treg requires the switching on and off of key genes that form part of the Treg gene regulatory network and raises the possibility that this is reversible. It is plausible that subtle shifts in expression levels of specific genes, including transcription factors and non-coding RNAs, change the regulation of the Treg gene network. The subtle skewing of gene expression initiates changes in function, with the potential to promote chronic disease and/or to license appropriate inflammatory responses. In the case of autoimmunity, there is an underlying genetic risk, and the interplay of genetic and environmental cues is complex and impacts gene regulation networks frequently involving promoters and enhancers, the regulatory elements that control gene expression levels and responsiveness. These promoter–enhancer interactions can operate over long distances and are highly cell type specific. In autoimmunity, the genetic risk can result in changes in these enhancer/promoter interactions, and this mainly impacts genes which are expressed in T cells and hence impacts Treg/conventional T-cell (Tconv) function. Genetic risk may cause the subtle alterations to the responsiveness of gene regulatory networks which are controlled by or control FOXP3 and its target genes, and the application of assays of the 3D organization of chromatin, enabling the connection of non-coding regulatory regions to the genes they control, is revealing the direct impact of environmental/metabolic/genetic risk on T-cell function and is providing mechanistic insight into susceptibility to inflammatory and autoimmune conditions.
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spelling pubmed-75336032020-10-15 Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease Brown, Cheryl Y. Sadlon, Timothy Hope, Christopher M. Wong, Ying Y. Wong, Soon Liu, Ning Withers, Holly Brown, Katherine Bandara, Veronika Gundsambuu, Batjargal Pederson, Stephen Breen, James Robertson, Sarah Anne Forrest, Alistair Beyer, Marc Barry, Simon Charles Front Immunol Immunology There has been much interest in the ability of regulatory T cells (Treg) to switch function in vivo, either as a result of genetic risk of disease or in response to environmental and metabolic cues. The relationship between levels of FOXP3 and functional fitness plays a significant part in this plasticity. There is an emerging role for Treg in tissue repair that may be less dependent on FOXP3, and the molecular mechanisms underpinning this are not fully understood. As a result of detailed, high-resolution functional genomics, the gene regulatory networks and key functional mediators of Treg phenotype downstream of FOXP3 have been mapped, enabling a mechanistic insight into Treg function. This transcription factor-driven programming of T-cell function to generate Treg requires the switching on and off of key genes that form part of the Treg gene regulatory network and raises the possibility that this is reversible. It is plausible that subtle shifts in expression levels of specific genes, including transcription factors and non-coding RNAs, change the regulation of the Treg gene network. The subtle skewing of gene expression initiates changes in function, with the potential to promote chronic disease and/or to license appropriate inflammatory responses. In the case of autoimmunity, there is an underlying genetic risk, and the interplay of genetic and environmental cues is complex and impacts gene regulation networks frequently involving promoters and enhancers, the regulatory elements that control gene expression levels and responsiveness. These promoter–enhancer interactions can operate over long distances and are highly cell type specific. In autoimmunity, the genetic risk can result in changes in these enhancer/promoter interactions, and this mainly impacts genes which are expressed in T cells and hence impacts Treg/conventional T-cell (Tconv) function. Genetic risk may cause the subtle alterations to the responsiveness of gene regulatory networks which are controlled by or control FOXP3 and its target genes, and the application of assays of the 3D organization of chromatin, enabling the connection of non-coding regulatory regions to the genes they control, is revealing the direct impact of environmental/metabolic/genetic risk on T-cell function and is providing mechanistic insight into susceptibility to inflammatory and autoimmune conditions. Frontiers Media S.A. 2020-09-15 /pmc/articles/PMC7533603/ /pubmed/33072063 http://dx.doi.org/10.3389/fimmu.2020.01269 Text en Copyright © 2020 Brown, Sadlon, Hope, Wong, Wong, Liu, Withers, Brown, Bandara, Gundsambuu, Pederson, Breen, Robertson, Forrest, Beyer and Barry. 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
Brown, Cheryl Y.
Sadlon, Timothy
Hope, Christopher M.
Wong, Ying Y.
Wong, Soon
Liu, Ning
Withers, Holly
Brown, Katherine
Bandara, Veronika
Gundsambuu, Batjargal
Pederson, Stephen
Breen, James
Robertson, Sarah Anne
Forrest, Alistair
Beyer, Marc
Barry, Simon Charles
Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title_full Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title_fullStr Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title_full_unstemmed Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title_short Molecular Insights Into Regulatory T-Cell Adaptation to Self, Environment, and Host Tissues: Plasticity or Loss of Function in Autoimmune Disease
title_sort molecular insights into regulatory t-cell adaptation to self, environment, and host tissues: plasticity or loss of function in autoimmune disease
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7533603/
https://www.ncbi.nlm.nih.gov/pubmed/33072063
http://dx.doi.org/10.3389/fimmu.2020.01269
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