The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.

Accurate genome duplication underlies genetic homeostasis. Metazoan Mdm2 binding protein (MTBP) forms a main regulatory platform for origin firing together with Treslin/TICRR and TopBP1 (Topoisomerase II binding protein 1 (TopBP1)-interacting replication stimulating protein/TopBP1-interacting checkp...

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Main Authors: Kerstin Köhler, Luis Sanchez-Pulido, Verena Höfer, Anika Marko, Chris P Ponting, Ambrosius P Snijders, Regina Feederle, Aloys Schepers, Dominik Boos
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-01-01
Series:PLoS Biology
Online Access:https://doi.org/10.1371/journal.pbio.2006767
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spelling doaj-cbe3c8776c044af9ab1fff82c10c7f322021-07-02T16:27:06ZengPublic Library of Science (PLoS)PLoS Biology1544-91731545-78852019-01-01171e200676710.1371/journal.pbio.2006767The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.Kerstin KöhlerLuis Sanchez-PulidoVerena HöferAnika MarkoChris P PontingAmbrosius P SnijdersRegina FeederleAloys SchepersDominik BoosAccurate genome duplication underlies genetic homeostasis. Metazoan Mdm2 binding protein (MTBP) forms a main regulatory platform for origin firing together with Treslin/TICRR and TopBP1 (Topoisomerase II binding protein 1 (TopBP1)-interacting replication stimulating protein/TopBP1-interacting checkpoint and replication regulator). We report the first comprehensive analysis of MTBP and reveal conserved and metazoa-specific MTBP functions in replication. This suggests that metazoa have evolved specific molecular mechanisms to adapt replication principles conserved with yeast to the specific requirements of the more complex metazoan cells. We uncover one such metazoa-specific process: a new replication factor, cyclin-dependent kinase 8/19-cyclinC (Cdk8/19-cyclin C), binds to a central domain of MTBP. This interaction is required for complete genome duplication in human cells. In the absence of MTBP binding to Cdk8/19-cyclin C, cells enter mitosis with incompletely duplicated chromosomes, and subsequent chromosome segregation occurs inaccurately. Using remote homology searches, we identified MTBP as the metazoan orthologue of yeast synthetic lethal with Dpb11 7 (Sld7). This homology finally demonstrates that the set of yeast core factors sufficient for replication initiation in vitro is conserved in metazoa. MTBP and Sld7 contain two homologous domains that are present in no other protein, one each in the N and C termini. In MTBP the conserved termini flank the metazoa-specific Cdk8/19-cyclin C binding region and are required for normal origin firing in human cells. The N termini of MTBP and Sld7 share an essential origin firing function, the interaction with Treslin/TICRR or its yeast orthologue Sld3, respectively. The C termini may function as homodimerisation domains. Our characterisation of broadly conserved and metazoa-specific initiation processes sets the basis for further mechanistic dissection of replication initiation in vertebrates. It is a first step in understanding the distinctions of origin firing in higher eukaryotes.https://doi.org/10.1371/journal.pbio.2006767
collection DOAJ
language English
format Article
sources DOAJ
author Kerstin Köhler
Luis Sanchez-Pulido
Verena Höfer
Anika Marko
Chris P Ponting
Ambrosius P Snijders
Regina Feederle
Aloys Schepers
Dominik Boos
spellingShingle Kerstin Köhler
Luis Sanchez-Pulido
Verena Höfer
Anika Marko
Chris P Ponting
Ambrosius P Snijders
Regina Feederle
Aloys Schepers
Dominik Boos
The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
PLoS Biology
author_facet Kerstin Köhler
Luis Sanchez-Pulido
Verena Höfer
Anika Marko
Chris P Ponting
Ambrosius P Snijders
Regina Feederle
Aloys Schepers
Dominik Boos
author_sort Kerstin Köhler
title The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
title_short The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
title_full The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
title_fullStr The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
title_full_unstemmed The Cdk8/19-cyclin C transcription regulator functions in genome replication through metazoan Sld7.
title_sort cdk8/19-cyclin c transcription regulator functions in genome replication through metazoan sld7.
publisher Public Library of Science (PLoS)
series PLoS Biology
issn 1544-9173
1545-7885
publishDate 2019-01-01
description Accurate genome duplication underlies genetic homeostasis. Metazoan Mdm2 binding protein (MTBP) forms a main regulatory platform for origin firing together with Treslin/TICRR and TopBP1 (Topoisomerase II binding protein 1 (TopBP1)-interacting replication stimulating protein/TopBP1-interacting checkpoint and replication regulator). We report the first comprehensive analysis of MTBP and reveal conserved and metazoa-specific MTBP functions in replication. This suggests that metazoa have evolved specific molecular mechanisms to adapt replication principles conserved with yeast to the specific requirements of the more complex metazoan cells. We uncover one such metazoa-specific process: a new replication factor, cyclin-dependent kinase 8/19-cyclinC (Cdk8/19-cyclin C), binds to a central domain of MTBP. This interaction is required for complete genome duplication in human cells. In the absence of MTBP binding to Cdk8/19-cyclin C, cells enter mitosis with incompletely duplicated chromosomes, and subsequent chromosome segregation occurs inaccurately. Using remote homology searches, we identified MTBP as the metazoan orthologue of yeast synthetic lethal with Dpb11 7 (Sld7). This homology finally demonstrates that the set of yeast core factors sufficient for replication initiation in vitro is conserved in metazoa. MTBP and Sld7 contain two homologous domains that are present in no other protein, one each in the N and C termini. In MTBP the conserved termini flank the metazoa-specific Cdk8/19-cyclin C binding region and are required for normal origin firing in human cells. The N termini of MTBP and Sld7 share an essential origin firing function, the interaction with Treslin/TICRR or its yeast orthologue Sld3, respectively. The C termini may function as homodimerisation domains. Our characterisation of broadly conserved and metazoa-specific initiation processes sets the basis for further mechanistic dissection of replication initiation in vertebrates. It is a first step in understanding the distinctions of origin firing in higher eukaryotes.
url https://doi.org/10.1371/journal.pbio.2006767
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