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Characteristics of Metazoan DNA Replication Origins

DNA replication in metazoan cells initiates at multiple discrete chromosomal sites called replication origins. Recent genome-wide studies have mapped thousands of origins in animal and plant cells, but without yielding a distinct and universal consensus sequence. However, origin-associated regions w...

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Autores principales: Hutchins, James R. A., Aze, Antoine, Coulombe, Philippe, Méchali, Marcel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7120227/
http://dx.doi.org/10.1007/978-4-431-55873-6_2
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author Hutchins, James R. A.
Aze, Antoine
Coulombe, Philippe
Méchali, Marcel
author_facet Hutchins, James R. A.
Aze, Antoine
Coulombe, Philippe
Méchali, Marcel
author_sort Hutchins, James R. A.
collection PubMed
description DNA replication in metazoan cells initiates at multiple discrete chromosomal sites called replication origins. Recent genome-wide studies have mapped thousands of origins in animal and plant cells, but without yielding a distinct and universal consensus sequence. However, origin-associated regions with particular base composition features have been identified, such as the G-rich OGRE motif, predicted to form G-quadruplexes. Epigenetic marks such as histone modifications that promote open chromatin also favor origin formation. Before DNA replication can initiate at origins, they need to be “licensed” by the binding of the origin recognition complex (ORC) and other proteins to form pre-replication and pre-initiation complexes. Origin-associated proteins are themselves subject to multilayered regulation, notably by posttranslational modification and proteasomal degradation. Origins are organized into replicons and replicon clusters, whose firing occurs at discrete subnuclear bodies known as replication foci. A still poorly characterized nuclear matrix structure might be involved in the attachment of replication units and the formation of replication foci. Preferential genomic sequences responsible for these attachments have been reported, as well as factors playing roles in their regulation. There appears to be great flexibility in the choice of origins used in each S-phase, being affected by factors including cell identity and replication stresses. Origin selection also changes dramatically during embryogenesis in concert with developmental signaling pathways. Dysregulation of origin positioning and recognition are implicated in human disease, as mutations in origin-binding proteins have been found in developmental disorders, and expansions in repeat-containing genomic regions promote genome instability. This chapter summarizes current understanding about replication origins, the most recent discoveries, and outlines key unanswered questions in this exciting field.
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spelling pubmed-71202272020-04-06 Characteristics of Metazoan DNA Replication Origins Hutchins, James R. A. Aze, Antoine Coulombe, Philippe Méchali, Marcel DNA Replication, Recombination, and Repair Article DNA replication in metazoan cells initiates at multiple discrete chromosomal sites called replication origins. Recent genome-wide studies have mapped thousands of origins in animal and plant cells, but without yielding a distinct and universal consensus sequence. However, origin-associated regions with particular base composition features have been identified, such as the G-rich OGRE motif, predicted to form G-quadruplexes. Epigenetic marks such as histone modifications that promote open chromatin also favor origin formation. Before DNA replication can initiate at origins, they need to be “licensed” by the binding of the origin recognition complex (ORC) and other proteins to form pre-replication and pre-initiation complexes. Origin-associated proteins are themselves subject to multilayered regulation, notably by posttranslational modification and proteasomal degradation. Origins are organized into replicons and replicon clusters, whose firing occurs at discrete subnuclear bodies known as replication foci. A still poorly characterized nuclear matrix structure might be involved in the attachment of replication units and the formation of replication foci. Preferential genomic sequences responsible for these attachments have been reported, as well as factors playing roles in their regulation. There appears to be great flexibility in the choice of origins used in each S-phase, being affected by factors including cell identity and replication stresses. Origin selection also changes dramatically during embryogenesis in concert with developmental signaling pathways. Dysregulation of origin positioning and recognition are implicated in human disease, as mutations in origin-binding proteins have been found in developmental disorders, and expansions in repeat-containing genomic regions promote genome instability. This chapter summarizes current understanding about replication origins, the most recent discoveries, and outlines key unanswered questions in this exciting field. 2015-09-25 /pmc/articles/PMC7120227/ http://dx.doi.org/10.1007/978-4-431-55873-6_2 Text en © Springer Japan 2016 This article is made available via the PMC Open Access Subset for unrestricted research re-use and secondary analysis in any form or by any means with acknowledgement of the original source. These permissions are granted for the duration of the World Health Organization (WHO) declaration of COVID-19 as a global pandemic.
spellingShingle Article
Hutchins, James R. A.
Aze, Antoine
Coulombe, Philippe
Méchali, Marcel
Characteristics of Metazoan DNA Replication Origins
title Characteristics of Metazoan DNA Replication Origins
title_full Characteristics of Metazoan DNA Replication Origins
title_fullStr Characteristics of Metazoan DNA Replication Origins
title_full_unstemmed Characteristics of Metazoan DNA Replication Origins
title_short Characteristics of Metazoan DNA Replication Origins
title_sort characteristics of metazoan dna replication origins
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7120227/
http://dx.doi.org/10.1007/978-4-431-55873-6_2
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