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Characterization of the replication timing program of 6 human model cell lines

During the S-phase, the DNA replication process is finely orchestrated and regulated by two programs: the spatial program that determines where replication will start in the genome (Cadoret et al. (2008 Oct 14), Cayrou et al. (2011 Sep), Picard et al. (2014 May 1) [1], [2], [3]), and the temporal pr...

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Autores principales: Hadjadj, Djihad, Denecker, Thomas, Maric, Chrystelle, Fauchereau, Fabien, Baldacci, Giuseppe, Cadoret, Jean-Charles
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961496/
https://www.ncbi.nlm.nih.gov/pubmed/27508120
http://dx.doi.org/10.1016/j.gdata.2016.07.003
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author Hadjadj, Djihad
Denecker, Thomas
Maric, Chrystelle
Fauchereau, Fabien
Baldacci, Giuseppe
Cadoret, Jean-Charles
author_facet Hadjadj, Djihad
Denecker, Thomas
Maric, Chrystelle
Fauchereau, Fabien
Baldacci, Giuseppe
Cadoret, Jean-Charles
author_sort Hadjadj, Djihad
collection PubMed
description During the S-phase, the DNA replication process is finely orchestrated and regulated by two programs: the spatial program that determines where replication will start in the genome (Cadoret et al. (2008 Oct 14), Cayrou et al. (2011 Sep), Picard et al. (2014 May 1) [1], [2], [3]), and the temporal program that determines when during the S phase different parts of the genome are replicated and when origins are activated. The temporal program is so well conserved for each cell type from independent individuals [4] that it is possible to identify a cell type from an unknown sample just by determining its replication timing program. Moreover, replicative domains are strongly correlated with the partition of the genome into topological domains (determined by the Hi-C method, Lieberman-Aiden et al. (2009 Oct 9), Pope et al. (2014 Nov 20) [5], [6]). On the one hand, replicative areas are well defined and participate in shaping the spatial organization of the genome for a given cell type. On the other hand, studies on the timing program during cell differentiation showed a certain plasticity of this program according to the stage of cell differentiation Hiratani et al. (2008 Oct 7, 2010 Feb) [7], [8]. Domains where a replication timing change was observed went through a nuclear re-localization. Thus the temporal program of replication can be considered as an epigenetic mark Hiratani and Gilbert (2009 Feb 16) [9]. We present the genomic data of replication timing in 6 human model cell lines: U2OS (GSM2111308), RKO (GSM2111309), HEK 293T (GSM2111310), HeLa (GSM2111311), MRC5-SV (GSM2111312) and K562 (GSM2111313). A short comparative analysis was performed that allowed us to define regions common to the 6 cell lines. These replication timing data can be taken into account when performing studies that use these model cell lines.
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spelling pubmed-49614962016-08-09 Characterization of the replication timing program of 6 human model cell lines Hadjadj, Djihad Denecker, Thomas Maric, Chrystelle Fauchereau, Fabien Baldacci, Giuseppe Cadoret, Jean-Charles Genom Data Data in Brief During the S-phase, the DNA replication process is finely orchestrated and regulated by two programs: the spatial program that determines where replication will start in the genome (Cadoret et al. (2008 Oct 14), Cayrou et al. (2011 Sep), Picard et al. (2014 May 1) [1], [2], [3]), and the temporal program that determines when during the S phase different parts of the genome are replicated and when origins are activated. The temporal program is so well conserved for each cell type from independent individuals [4] that it is possible to identify a cell type from an unknown sample just by determining its replication timing program. Moreover, replicative domains are strongly correlated with the partition of the genome into topological domains (determined by the Hi-C method, Lieberman-Aiden et al. (2009 Oct 9), Pope et al. (2014 Nov 20) [5], [6]). On the one hand, replicative areas are well defined and participate in shaping the spatial organization of the genome for a given cell type. On the other hand, studies on the timing program during cell differentiation showed a certain plasticity of this program according to the stage of cell differentiation Hiratani et al. (2008 Oct 7, 2010 Feb) [7], [8]. Domains where a replication timing change was observed went through a nuclear re-localization. Thus the temporal program of replication can be considered as an epigenetic mark Hiratani and Gilbert (2009 Feb 16) [9]. We present the genomic data of replication timing in 6 human model cell lines: U2OS (GSM2111308), RKO (GSM2111309), HEK 293T (GSM2111310), HeLa (GSM2111311), MRC5-SV (GSM2111312) and K562 (GSM2111313). A short comparative analysis was performed that allowed us to define regions common to the 6 cell lines. These replication timing data can be taken into account when performing studies that use these model cell lines. Elsevier 2016-07-15 /pmc/articles/PMC4961496/ /pubmed/27508120 http://dx.doi.org/10.1016/j.gdata.2016.07.003 Text en © 2016 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Data in Brief
Hadjadj, Djihad
Denecker, Thomas
Maric, Chrystelle
Fauchereau, Fabien
Baldacci, Giuseppe
Cadoret, Jean-Charles
Characterization of the replication timing program of 6 human model cell lines
title Characterization of the replication timing program of 6 human model cell lines
title_full Characterization of the replication timing program of 6 human model cell lines
title_fullStr Characterization of the replication timing program of 6 human model cell lines
title_full_unstemmed Characterization of the replication timing program of 6 human model cell lines
title_short Characterization of the replication timing program of 6 human model cell lines
title_sort characterization of the replication timing program of 6 human model cell lines
topic Data in Brief
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961496/
https://www.ncbi.nlm.nih.gov/pubmed/27508120
http://dx.doi.org/10.1016/j.gdata.2016.07.003
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