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PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C

Polycomb group proteins (PcG) exert conserved epigenetic functions that convey maintenance of repressed transcriptional states, via post-translational histone modifications and high order structure formation. During S-phase, in order to preserve cell identity, in addition to DNA information, PcG-chr...

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Detalles Bibliográficos
Autores principales: Lo Sardo, Federica, Lanzuolo, Chiara, Comoglio, Federico, De Bardi, Marco, Paro, Renato, Orlando, Valerio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3578750/
https://www.ncbi.nlm.nih.gov/pubmed/23437006
http://dx.doi.org/10.1371/journal.pgen.1003283
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author Lo Sardo, Federica
Lanzuolo, Chiara
Comoglio, Federico
De Bardi, Marco
Paro, Renato
Orlando, Valerio
author_facet Lo Sardo, Federica
Lanzuolo, Chiara
Comoglio, Federico
De Bardi, Marco
Paro, Renato
Orlando, Valerio
author_sort Lo Sardo, Federica
collection PubMed
description Polycomb group proteins (PcG) exert conserved epigenetic functions that convey maintenance of repressed transcriptional states, via post-translational histone modifications and high order structure formation. During S-phase, in order to preserve cell identity, in addition to DNA information, PcG-chromatin-mediated epigenetic signatures need to be duplicated requiring a tight coordination between PcG proteins and replication programs. However, the interconnection between replication timing control and PcG functions remains unknown. Using Drosophila embryonic cell lines, we find that, while presence of specific PcG complexes and underlying transcription state are not the sole determinants of cellular replication timing, PcG-mediated higher-order structures appear to dictate the timing of replication and maintenance of the silenced state. Using published datasets we show that PRC1, PRC2, and PhoRC complexes differently correlate with replication timing of their targets. In the fully repressed BX-C, loss of function experiments revealed a synergistic role for PcG proteins in the maintenance of replication programs through the mediation of higher-order structures. Accordingly, replication timing analysis performed on two Drosophila cell lines differing for BX-C gene expression states, PcG distribution, and chromatin domain conformation revealed a cell-type-specific replication program that mirrors lineage-specific BX-C higher-order structures. Our work suggests that PcG complexes, by regulating higher-order chromatin structure at their target sites, contribute to the definition and the maintenance of genomic structural domains where genes showing the same epigenetic state replicate at the same time.
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spelling pubmed-35787502013-02-22 PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C Lo Sardo, Federica Lanzuolo, Chiara Comoglio, Federico De Bardi, Marco Paro, Renato Orlando, Valerio PLoS Genet Research Article Polycomb group proteins (PcG) exert conserved epigenetic functions that convey maintenance of repressed transcriptional states, via post-translational histone modifications and high order structure formation. During S-phase, in order to preserve cell identity, in addition to DNA information, PcG-chromatin-mediated epigenetic signatures need to be duplicated requiring a tight coordination between PcG proteins and replication programs. However, the interconnection between replication timing control and PcG functions remains unknown. Using Drosophila embryonic cell lines, we find that, while presence of specific PcG complexes and underlying transcription state are not the sole determinants of cellular replication timing, PcG-mediated higher-order structures appear to dictate the timing of replication and maintenance of the silenced state. Using published datasets we show that PRC1, PRC2, and PhoRC complexes differently correlate with replication timing of their targets. In the fully repressed BX-C, loss of function experiments revealed a synergistic role for PcG proteins in the maintenance of replication programs through the mediation of higher-order structures. Accordingly, replication timing analysis performed on two Drosophila cell lines differing for BX-C gene expression states, PcG distribution, and chromatin domain conformation revealed a cell-type-specific replication program that mirrors lineage-specific BX-C higher-order structures. Our work suggests that PcG complexes, by regulating higher-order chromatin structure at their target sites, contribute to the definition and the maintenance of genomic structural domains where genes showing the same epigenetic state replicate at the same time. Public Library of Science 2013-02-21 /pmc/articles/PMC3578750/ /pubmed/23437006 http://dx.doi.org/10.1371/journal.pgen.1003283 Text en © 2013 Lo Sardo 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
Lo Sardo, Federica
Lanzuolo, Chiara
Comoglio, Federico
De Bardi, Marco
Paro, Renato
Orlando, Valerio
PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title_full PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title_fullStr PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title_full_unstemmed PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title_short PcG-Mediated Higher-Order Chromatin Structures Modulate Replication Programs at the Drosophila BX-C
title_sort pcg-mediated higher-order chromatin structures modulate replication programs at the drosophila bx-c
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3578750/
https://www.ncbi.nlm.nih.gov/pubmed/23437006
http://dx.doi.org/10.1371/journal.pgen.1003283
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