Developmental differences in genome replication program and origin activation

dc.contributor.author Rausch, Cathia
dc.contributor.author Weber, Patrick
dc.contributor.author Prorok, Paulina
dc.contributor.author Hörl, David
dc.contributor.author Maiser, Andreas
dc.contributor.author Lehmkuhl, Anne
dc.contributor.author Chagin, Vadim O.
dc.contributor.author Casas-Delucchi, Corella S
dc.contributor.author Leonhardt, Heinrich
dc.contributor.author Cardoso, M. Cristina
dc.date.accessioned 2020-06-30T14:42:59Z
dc.date.available 2020-06-30T14:42:59Z
dc.date.created 2020-06-30
dc.date.issued 2020-06-30
dc.description To ensure error-free duplication of all (epi)genetic information once per cell cycle, DNA replication follows a cell type and developmental stage specific spatio-temporal program. Here, we analyze the spatio-temporal DNA replication progression in (un)differentiated mouse embryonic stem (mES) cells. Whereas telomeres replicate throughout S-phase, we observe mid-S phase replication of (peri)centromeric heterochromatin in mES cells, which switches to late S-phase replication upon differentiation correlating with increase in condensation and decrease in acetylation of chromatin. We also find synchronous duplication of the Y chromosome, marking the end of S-phase, irrespectively of the pluripotency state. Using a combination of single-molecule and super-resolution microscopy, we measure molecular properties of the mES cell replicon, the number of replication foci active in parallel and their spatial clustering in mES cells versus somatic cells. We conclude that each replication nanofocus in mES cells corresponds to an individual replicon, with approximately up to one quarter representing unidirectional forks. Furthermore, with molecular combing and genome-wide origin mapping analyses we find that mES cells activate twice as many origins spaced at half the distance than somatic cells. Altogether, our results highlight fundamental developmental differences on progression of genome replication and origin activation in pluripotent cells. en_US
dc.identifier.uri https://tudatalib.ulb.tu-darmstadt.de/handle/tudatalib/2376
dc.identifier.uri https://doi.org/10.25534/tudatalib-220
dc.language.iso en en_US
dc.rights.licenseCC-BY-NC-4.0 (https://creativecommons.org/licenses/by-nc/4.0)
dc.subject DNA replication en_US
dc.subject origin activation en_US
dc.subject replication timing en_US
dc.subject embryonic stem cells en_US
dc.subject.classification 2.11-03
dc.subject.ddc 570
dc.title Developmental differences in genome replication program and origin activation en_US
dc.type Text en_US
dc.type Software en_US
dc.type Image en_US
dcterms.accessRights openAccess
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person.identifier.orcid 0000-0003-1710-1708
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person.identifier.orcid 0000-0003-2531-1123
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tuda.history.classification Version=2020-2024;201-03 Zellbiologie
tuda.project DFG | CA198/9-2 | Hochauflösende Analy
tuda.project DFG | CA198/12-1 | Einfluss von DNA-Bas
tuda.project DFG | SFB1361,TP06 | TP_06_Cardoso_Mainz

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