Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription

Differentiation-dependent regulation of the Ifng cytokine gene locus in T helper (Th) cells has emerged as an excellent model for functional study of distal elements that control lineage-specific gene expression. We previously identified a cis-regulatory element located 22 kb upstream of the Ifng ge...

Descripción completa

Detalles Bibliográficos
Autores principales: Balasubramani, Anand, Winstead, Colleen J., Turner, Henrietta, Janowski, Karen M., Harbour, Stacey N., Shibata, Yoichiro, Crawford, Gregory E., Hatton, Robin D., Weaver, Casey T.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3886902/
https://www.ncbi.nlm.nih.gov/pubmed/24415943
http://dx.doi.org/10.1371/journal.pgen.1003969
_version_ 1782478931816873984
author Balasubramani, Anand
Winstead, Colleen J.
Turner, Henrietta
Janowski, Karen M.
Harbour, Stacey N.
Shibata, Yoichiro
Crawford, Gregory E.
Hatton, Robin D.
Weaver, Casey T.
author_facet Balasubramani, Anand
Winstead, Colleen J.
Turner, Henrietta
Janowski, Karen M.
Harbour, Stacey N.
Shibata, Yoichiro
Crawford, Gregory E.
Hatton, Robin D.
Weaver, Casey T.
author_sort Balasubramani, Anand
collection PubMed
description Differentiation-dependent regulation of the Ifng cytokine gene locus in T helper (Th) cells has emerged as an excellent model for functional study of distal elements that control lineage-specific gene expression. We previously identified a cis-regulatory element located 22 kb upstream of the Ifng gene (Conserved Non-coding Sequence -22, or CNS-22) that is a site for recruitment of the transcription factors T-bet, Runx3, NF-κB and STAT4, which act to regulate transcription of the Ifng gene in Th1 cells. Here, we report the generation of mice with a conditional deletion of CNS-22 that has enabled us to define the epigenetic and functional consequences of its absence. Deletion of CNS-22 led to a defect in induction of Ifng by the cytokines IL-12 and IL-18, with a more modest effect on induction via T-cell receptor activation. To better understand how CNS-22 and other Ifng CNSs regulated Ifng transcription in response to these distinct stimuli, we examined activation-dependent changes in epigenetic modifications across the extended Ifng locus in CNS-22-deficient T cells. We demonstrate that in response to both cytokine and TCR driven activation signals, CNS-22 and other Ifng CNSs recruit increased activity of histone acetyl transferases (HATs) that transiently enhance levels of histones H3 and H4 acetylation across the extended Ifng locus. We also demonstrate that activation-responsive increases in histone acetylation levels are directly linked to the ability of Ifng CNSs to acutely enhance Pol II recruitment to the Ifng promoter. Finally, we show that impairment in IL-12+IL-18 dependent induction of Ifng stems from the importance of CNS-22 in coordinating locus-wide levels of histone acetylation in response to these cytokines. These findings identify a role for acute histone acetylation in the enhancer function of distal conserved cis-elements that regulate of Ifng gene expression.
format Online
Article
Text
id pubmed-3886902
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-38869022014-01-10 Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription Balasubramani, Anand Winstead, Colleen J. Turner, Henrietta Janowski, Karen M. Harbour, Stacey N. Shibata, Yoichiro Crawford, Gregory E. Hatton, Robin D. Weaver, Casey T. PLoS Genet Research Article Differentiation-dependent regulation of the Ifng cytokine gene locus in T helper (Th) cells has emerged as an excellent model for functional study of distal elements that control lineage-specific gene expression. We previously identified a cis-regulatory element located 22 kb upstream of the Ifng gene (Conserved Non-coding Sequence -22, or CNS-22) that is a site for recruitment of the transcription factors T-bet, Runx3, NF-κB and STAT4, which act to regulate transcription of the Ifng gene in Th1 cells. Here, we report the generation of mice with a conditional deletion of CNS-22 that has enabled us to define the epigenetic and functional consequences of its absence. Deletion of CNS-22 led to a defect in induction of Ifng by the cytokines IL-12 and IL-18, with a more modest effect on induction via T-cell receptor activation. To better understand how CNS-22 and other Ifng CNSs regulated Ifng transcription in response to these distinct stimuli, we examined activation-dependent changes in epigenetic modifications across the extended Ifng locus in CNS-22-deficient T cells. We demonstrate that in response to both cytokine and TCR driven activation signals, CNS-22 and other Ifng CNSs recruit increased activity of histone acetyl transferases (HATs) that transiently enhance levels of histones H3 and H4 acetylation across the extended Ifng locus. We also demonstrate that activation-responsive increases in histone acetylation levels are directly linked to the ability of Ifng CNSs to acutely enhance Pol II recruitment to the Ifng promoter. Finally, we show that impairment in IL-12+IL-18 dependent induction of Ifng stems from the importance of CNS-22 in coordinating locus-wide levels of histone acetylation in response to these cytokines. These findings identify a role for acute histone acetylation in the enhancer function of distal conserved cis-elements that regulate of Ifng gene expression. Public Library of Science 2014-01-09 /pmc/articles/PMC3886902/ /pubmed/24415943 http://dx.doi.org/10.1371/journal.pgen.1003969 Text en © 2014 Balasubramani et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Balasubramani, Anand
Winstead, Colleen J.
Turner, Henrietta
Janowski, Karen M.
Harbour, Stacey N.
Shibata, Yoichiro
Crawford, Gregory E.
Hatton, Robin D.
Weaver, Casey T.
Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title_full Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title_fullStr Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title_full_unstemmed Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title_short Deletion of a Conserved cis-Element in the Ifng Locus Highlights the Role of Acute Histone Acetylation in Modulating Inducible Gene Transcription
title_sort deletion of a conserved cis-element in the ifng locus highlights the role of acute histone acetylation in modulating inducible gene transcription
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3886902/
https://www.ncbi.nlm.nih.gov/pubmed/24415943
http://dx.doi.org/10.1371/journal.pgen.1003969
work_keys_str_mv AT balasubramanianand deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT winsteadcolleenj deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT turnerhenrietta deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT janowskikarenm deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT harbourstaceyn deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT shibatayoichiro deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT crawfordgregorye deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT hattonrobind deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription
AT weavercaseyt deletionofaconservedciselementintheifnglocushighlightstheroleofacutehistoneacetylationinmodulatinginduciblegenetranscription

Ejemplares similares