Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome

Genome-wide replication timing studies have suggested that mammalian chromosomes consist of megabase-scale domains of coordinated origin firing separated by large originless transition regions. Here, we report a quantitative genome-wide analysis of DNA replication kinetics in several human cell type...

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Autores principales: Guilbaud, Guillaume, Rappailles, Aurélien, Baker, Antoine, Chen, Chun-Long, Arneodo, Alain, Goldar, Arach, d'Aubenton-Carafa, Yves, Thermes, Claude, Audit, Benjamin, Hyrien, Olivier
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3248390/
https://www.ncbi.nlm.nih.gov/pubmed/22219720
http://dx.doi.org/10.1371/journal.pcbi.1002322
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author Guilbaud, Guillaume
Rappailles, Aurélien
Baker, Antoine
Chen, Chun-Long
Arneodo, Alain
Goldar, Arach
d'Aubenton-Carafa, Yves
Thermes, Claude
Audit, Benjamin
Hyrien, Olivier
author_facet Guilbaud, Guillaume
Rappailles, Aurélien
Baker, Antoine
Chen, Chun-Long
Arneodo, Alain
Goldar, Arach
d'Aubenton-Carafa, Yves
Thermes, Claude
Audit, Benjamin
Hyrien, Olivier
author_sort Guilbaud, Guillaume
collection PubMed
description Genome-wide replication timing studies have suggested that mammalian chromosomes consist of megabase-scale domains of coordinated origin firing separated by large originless transition regions. Here, we report a quantitative genome-wide analysis of DNA replication kinetics in several human cell types that contradicts this view. DNA combing in HeLa cells sorted into four temporal compartments of S phase shows that replication origins are spaced at 40 kb intervals and fire as small clusters whose synchrony increases during S phase and that replication fork velocity (mean 0.7 kb/min, maximum 2.0 kb/min) remains constant and narrowly distributed through S phase. However, multi-scale analysis of a genome-wide replication timing profile shows a broad distribution of replication timing gradients with practically no regions larger than 100 kb replicating at less than 2 kb/min. Therefore, HeLa cells lack large regions of unidirectional fork progression. Temporal transition regions are replicated by sequential activation of origins at a rate that increases during S phase and replication timing gradients are set by the delay and the spacing between successive origin firings rather than by the velocity of single forks. Activation of internal origins in a specific temporal transition region is directly demonstrated by DNA combing of the IGH locus in HeLa cells. Analysis of published origin maps in HeLa cells and published replication timing and DNA combing data in several other cell types corroborate these findings, with the interesting exception of embryonic stem cells where regions of unidirectional fork progression seem more abundant. These results can be explained if origins fire independently of each other but under the control of long-range chromatin structure, or if replication forks progressing from early origins stimulate initiation in nearby unreplicated DNA. These findings shed a new light on the replication timing program of mammalian genomes and provide a general model for their replication kinetics.
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spelling pubmed-32483902012-01-04 Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome Guilbaud, Guillaume Rappailles, Aurélien Baker, Antoine Chen, Chun-Long Arneodo, Alain Goldar, Arach d'Aubenton-Carafa, Yves Thermes, Claude Audit, Benjamin Hyrien, Olivier PLoS Comput Biol Research Article Genome-wide replication timing studies have suggested that mammalian chromosomes consist of megabase-scale domains of coordinated origin firing separated by large originless transition regions. Here, we report a quantitative genome-wide analysis of DNA replication kinetics in several human cell types that contradicts this view. DNA combing in HeLa cells sorted into four temporal compartments of S phase shows that replication origins are spaced at 40 kb intervals and fire as small clusters whose synchrony increases during S phase and that replication fork velocity (mean 0.7 kb/min, maximum 2.0 kb/min) remains constant and narrowly distributed through S phase. However, multi-scale analysis of a genome-wide replication timing profile shows a broad distribution of replication timing gradients with practically no regions larger than 100 kb replicating at less than 2 kb/min. Therefore, HeLa cells lack large regions of unidirectional fork progression. Temporal transition regions are replicated by sequential activation of origins at a rate that increases during S phase and replication timing gradients are set by the delay and the spacing between successive origin firings rather than by the velocity of single forks. Activation of internal origins in a specific temporal transition region is directly demonstrated by DNA combing of the IGH locus in HeLa cells. Analysis of published origin maps in HeLa cells and published replication timing and DNA combing data in several other cell types corroborate these findings, with the interesting exception of embryonic stem cells where regions of unidirectional fork progression seem more abundant. These results can be explained if origins fire independently of each other but under the control of long-range chromatin structure, or if replication forks progressing from early origins stimulate initiation in nearby unreplicated DNA. These findings shed a new light on the replication timing program of mammalian genomes and provide a general model for their replication kinetics. Public Library of Science 2011-12-29 /pmc/articles/PMC3248390/ /pubmed/22219720 http://dx.doi.org/10.1371/journal.pcbi.1002322 Text en Guilbaud 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
Guilbaud, Guillaume
Rappailles, Aurélien
Baker, Antoine
Chen, Chun-Long
Arneodo, Alain
Goldar, Arach
d'Aubenton-Carafa, Yves
Thermes, Claude
Audit, Benjamin
Hyrien, Olivier
Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title_full Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title_fullStr Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title_full_unstemmed Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title_short Evidence for Sequential and Increasing Activation of Replication Origins along Replication Timing Gradients in the Human Genome
title_sort evidence for sequential and increasing activation of replication origins along replication timing gradients in the human genome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3248390/
https://www.ncbi.nlm.nih.gov/pubmed/22219720
http://dx.doi.org/10.1371/journal.pcbi.1002322
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