CDK contribution to DSB formation and recombination in fission yeast meiosis

CDKs (cyclin-dependent kinases) associate with different cyclins to form different CDK-complexes that are fundamental for an ordered cell cycle progression, and the coordination of this progression with different aspects of the cellular physiology. During meiosis programmed DNA double-strand breaks...

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Autores principales: Bustamante-Jaramillo, Luisa F., Ramos, Celia, Alonso, Leticia, Sesmero, Aroa, Segurado, Mónica, Martín-Castellanos, Cristina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6331086/
https://www.ncbi.nlm.nih.gov/pubmed/30640914
http://dx.doi.org/10.1371/journal.pgen.1007876
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author Bustamante-Jaramillo, Luisa F.
Ramos, Celia
Alonso, Leticia
Sesmero, Aroa
Segurado, Mónica
Martín-Castellanos, Cristina
author_facet Bustamante-Jaramillo, Luisa F.
Ramos, Celia
Alonso, Leticia
Sesmero, Aroa
Segurado, Mónica
Martín-Castellanos, Cristina
author_sort Bustamante-Jaramillo, Luisa F.
collection PubMed
description CDKs (cyclin-dependent kinases) associate with different cyclins to form different CDK-complexes that are fundamental for an ordered cell cycle progression, and the coordination of this progression with different aspects of the cellular physiology. During meiosis programmed DNA double-strand breaks (DSBs) initiate recombination that in addition to generating genetic variability are essential for the reductional chromosome segregation during the first meiotic division, and therefore for genome stability and viability of the gametes. However, how meiotic progression and DSB formation are coordinated, and the role CDKs have in the process, is not well understood. We have used single and double cyclin deletion mutants, and chemical inhibition of global CDK activity using the cdc2-asM17 allele, to address the requirement of CDK activity for DSB formation and recombination in fission yeast. We report that several cyclins (Cig1, Cig2, and the meiosis-specific Crs1) control DSB formation and recombination, with a major contribution of Crs1. Moreover, complementation analysis indicates specificity at least for this cyclin, suggesting that different CDK complexes might act in different pathways to promote recombination. Down-regulation of CDK activity impinges on the formation of linear elements (LinEs, protein complexes required for break formation at most DSB hotspot sites). This defect correlates with a reduction in the capability of one structural component (Rec25) to bind chromatin, suggesting a molecular mechanism by which CDK controls break formation. However, reduction in DSB formation in cyclin deletion mutants does not always correspondingly correlate with a proportional reduction in meiotic recombination (crossovers), suggesting that specific CDK complexes might also control downstream events balancing repair pathways. Therefore, our work points to CDK regulation of DSB formation as a key conserved feature in the initiation of meiotic recombination, in addition to provide a view of possible roles CDK might have in other steps of the recombination process.
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spelling pubmed-63310862019-02-01 CDK contribution to DSB formation and recombination in fission yeast meiosis Bustamante-Jaramillo, Luisa F. Ramos, Celia Alonso, Leticia Sesmero, Aroa Segurado, Mónica Martín-Castellanos, Cristina PLoS Genet Research Article CDKs (cyclin-dependent kinases) associate with different cyclins to form different CDK-complexes that are fundamental for an ordered cell cycle progression, and the coordination of this progression with different aspects of the cellular physiology. During meiosis programmed DNA double-strand breaks (DSBs) initiate recombination that in addition to generating genetic variability are essential for the reductional chromosome segregation during the first meiotic division, and therefore for genome stability and viability of the gametes. However, how meiotic progression and DSB formation are coordinated, and the role CDKs have in the process, is not well understood. We have used single and double cyclin deletion mutants, and chemical inhibition of global CDK activity using the cdc2-asM17 allele, to address the requirement of CDK activity for DSB formation and recombination in fission yeast. We report that several cyclins (Cig1, Cig2, and the meiosis-specific Crs1) control DSB formation and recombination, with a major contribution of Crs1. Moreover, complementation analysis indicates specificity at least for this cyclin, suggesting that different CDK complexes might act in different pathways to promote recombination. Down-regulation of CDK activity impinges on the formation of linear elements (LinEs, protein complexes required for break formation at most DSB hotspot sites). This defect correlates with a reduction in the capability of one structural component (Rec25) to bind chromatin, suggesting a molecular mechanism by which CDK controls break formation. However, reduction in DSB formation in cyclin deletion mutants does not always correspondingly correlate with a proportional reduction in meiotic recombination (crossovers), suggesting that specific CDK complexes might also control downstream events balancing repair pathways. Therefore, our work points to CDK regulation of DSB formation as a key conserved feature in the initiation of meiotic recombination, in addition to provide a view of possible roles CDK might have in other steps of the recombination process. Public Library of Science 2019-01-14 /pmc/articles/PMC6331086/ /pubmed/30640914 http://dx.doi.org/10.1371/journal.pgen.1007876 Text en © 2019 Bustamante-Jaramillo 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Bustamante-Jaramillo, Luisa F.
Ramos, Celia
Alonso, Leticia
Sesmero, Aroa
Segurado, Mónica
Martín-Castellanos, Cristina
CDK contribution to DSB formation and recombination in fission yeast meiosis
title CDK contribution to DSB formation and recombination in fission yeast meiosis
title_full CDK contribution to DSB formation and recombination in fission yeast meiosis
title_fullStr CDK contribution to DSB formation and recombination in fission yeast meiosis
title_full_unstemmed CDK contribution to DSB formation and recombination in fission yeast meiosis
title_short CDK contribution to DSB formation and recombination in fission yeast meiosis
title_sort cdk contribution to dsb formation and recombination in fission yeast meiosis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6331086/
https://www.ncbi.nlm.nih.gov/pubmed/30640914
http://dx.doi.org/10.1371/journal.pgen.1007876
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