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Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency

The genome of pluripotent stem cells adopts a unique three-dimensional architecture featuring weakly condensed heterochromatin and large nucleosome-free regions. Yet, it is unknown whether structural loops and contact domains display characteristics that distinguish embryonic stem cells (ESCs) from...

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Autores principales: Pękowska, Aleksandra, Klaus, Bernd, Xiang, Wanqing, Severino, Jacqueline, Daigle, Nathalie, Klein, Felix A., Oleś, Małgorzata, Casellas, Rafael, Ellenberg, Jan, Steinmetz, Lars M., Bertone, Paul, Huber, Wolfgang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6327227/
https://www.ncbi.nlm.nih.gov/pubmed/30414923
http://dx.doi.org/10.1016/j.cels.2018.09.003
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author Pękowska, Aleksandra
Klaus, Bernd
Xiang, Wanqing
Severino, Jacqueline
Daigle, Nathalie
Klein, Felix A.
Oleś, Małgorzata
Casellas, Rafael
Ellenberg, Jan
Steinmetz, Lars M.
Bertone, Paul
Huber, Wolfgang
author_facet Pękowska, Aleksandra
Klaus, Bernd
Xiang, Wanqing
Severino, Jacqueline
Daigle, Nathalie
Klein, Felix A.
Oleś, Małgorzata
Casellas, Rafael
Ellenberg, Jan
Steinmetz, Lars M.
Bertone, Paul
Huber, Wolfgang
author_sort Pękowska, Aleksandra
collection PubMed
description The genome of pluripotent stem cells adopts a unique three-dimensional architecture featuring weakly condensed heterochromatin and large nucleosome-free regions. Yet, it is unknown whether structural loops and contact domains display characteristics that distinguish embryonic stem cells (ESCs) from differentiated cell types. We used genome-wide chromosome conformation capture and super-resolution imaging to determine nuclear organization in mouse ESC and neural stem cell (NSC) derivatives. We found that loss of pluripotency is accompanied by widespread gain of structural loops. This general architectural change correlates with enhanced binding of CTCF and cohesins and more pronounced insulation of contacts across chromatin boundaries in lineage-committed cells. Reprogramming NSCs to pluripotency restores the unique features of ESC domain topology. Domains defined by the anchors of loops established upon differentiation are enriched for developmental genes. Chromatin loop formation is a pervasive structural alteration to the genome that accompanies exit from pluripotency and delineates the spatial segregation of developmentally regulated genes.
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spelling pubmed-63272272019-01-18 Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency Pękowska, Aleksandra Klaus, Bernd Xiang, Wanqing Severino, Jacqueline Daigle, Nathalie Klein, Felix A. Oleś, Małgorzata Casellas, Rafael Ellenberg, Jan Steinmetz, Lars M. Bertone, Paul Huber, Wolfgang Cell Syst Article The genome of pluripotent stem cells adopts a unique three-dimensional architecture featuring weakly condensed heterochromatin and large nucleosome-free regions. Yet, it is unknown whether structural loops and contact domains display characteristics that distinguish embryonic stem cells (ESCs) from differentiated cell types. We used genome-wide chromosome conformation capture and super-resolution imaging to determine nuclear organization in mouse ESC and neural stem cell (NSC) derivatives. We found that loss of pluripotency is accompanied by widespread gain of structural loops. This general architectural change correlates with enhanced binding of CTCF and cohesins and more pronounced insulation of contacts across chromatin boundaries in lineage-committed cells. Reprogramming NSCs to pluripotency restores the unique features of ESC domain topology. Domains defined by the anchors of loops established upon differentiation are enriched for developmental genes. Chromatin loop formation is a pervasive structural alteration to the genome that accompanies exit from pluripotency and delineates the spatial segregation of developmentally regulated genes. Cell Press 2018-11-28 /pmc/articles/PMC6327227/ /pubmed/30414923 http://dx.doi.org/10.1016/j.cels.2018.09.003 Text en http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Pękowska, Aleksandra
Klaus, Bernd
Xiang, Wanqing
Severino, Jacqueline
Daigle, Nathalie
Klein, Felix A.
Oleś, Małgorzata
Casellas, Rafael
Ellenberg, Jan
Steinmetz, Lars M.
Bertone, Paul
Huber, Wolfgang
Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title_full Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title_fullStr Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title_full_unstemmed Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title_short Gain of CTCF-Anchored Chromatin Loops Marks the Exit from Naive Pluripotency
title_sort gain of ctcf-anchored chromatin loops marks the exit from naive pluripotency
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6327227/
https://www.ncbi.nlm.nih.gov/pubmed/30414923
http://dx.doi.org/10.1016/j.cels.2018.09.003
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