Publikation: DEK oncoprotein participates in heterochromatin replication via SUMO-dependent nuclear bodies
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Datum
2023
Autor:innen
Pierzynska-Mach, Agnieszka
Osswald, Xenia
Bartoschek, Denis
Diaspro, Alberto
Kappes, Ferdinand
Herausgeber:innen
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European Union (EU): 841661
Deutsche Forschungsgemeinschaft (DFG): RTG1331
Deutsche Forschungsgemeinschaft (DFG): CRC969
Deutsche Forschungsgemeinschaft: CRC969
Deutsche Forschungsgemeinschaft (DFG): RTG1331
Deutsche Forschungsgemeinschaft (DFG): CRC969
Deutsche Forschungsgemeinschaft: CRC969
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Open Access-Veröffentlichung
Open Access Hybrid
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Core Facility der Universität Konstanz
Bioimaging Centre
Titel in einer weiteren Sprache
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Published
Erschienen in
Journal of Cell Science. The Company of Biologists. 2023, 136(23), jcs261329. ISSN 0021-9533. eISSN 1477-9137. Verfügbar unter: doi: 10.1242/jcs.261329
Zusammenfassung
The correct inheritance of chromatin structure is key for maintaining genome function and cell identity and preventing cellular transformation. DEK, a conserved non-histone chromatin protein, has recognized tumor-promoting properties, its overexpression being associated with poor prognosis in various cancer types. At the cellular level, DEK displays pleiotropic functions, influencing differentiation, apoptosis and stemness, but a characteristic oncogenic mechanism has remained elusive. Here, we report the identification of DEK bodies, focal assemblies of DEK that regularly occur at specific, yet unidentified, sites of heterochromatin replication exclusively in late S-phase. In these bodies, DEK localizes in direct proximity to active replisomes in agreement with a function in the early maturation of heterochromatin. A high-throughput siRNA screen, supported by mutational and biochemical analyses, identifies SUMO as one regulator of DEK body formation, linking DEK to the complex SUMO protein network that controls chromatin states and cell fate. This work combines and refines our previous data on DEK as a factor essential for heterochromatin integrity and facilitating replication under stress, and delineates an avenue of further study for unraveling the contribution of DEK to cancer development.
Zusammenfassung in einer weiteren Sprache
Fachgebiet (DDC)
570 Biowissenschaften, Biologie
Schlagwörter
Oncogene, Breast cancer, Replication stress, Histone modification, Superresolution microscopy, siRNA screen
Konferenz
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ISO 690
PIERZYNSKA-MACH, Agnieszka, Christina CZADA, Christopher VOGEL, Eva GWOSCH, Xenia OSSWALD, Denis BARTOSCHEK, Alberto DIASPRO, Ferdinand KAPPES, Elisa FERRANDO-MAY, 2023. DEK oncoprotein participates in heterochromatin replication via SUMO-dependent nuclear bodies. In: Journal of Cell Science. The Company of Biologists. 2023, 136(23), jcs261329. ISSN 0021-9533. eISSN 1477-9137. Verfügbar unter: doi: 10.1242/jcs.261329BibTex
@article{PierzynskaMach2023-12-01oncop-69560,
year={2023},
doi={10.1242/jcs.261329},
title={DEK oncoprotein participates in heterochromatin replication via SUMO-dependent nuclear bodies},
number={23},
volume={136},
issn={0021-9533},
journal={Journal of Cell Science},
author={Pierzynska-Mach, Agnieszka and Czada, Christina and Vogel, Christopher and Gwosch, Eva and Osswald, Xenia and Bartoschek, Denis and Diaspro, Alberto and Kappes, Ferdinand and Ferrando-May, Elisa},
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<dcterms:abstract>The correct inheritance of chromatin structure is key for maintaining genome function and cell identity and preventing cellular transformation. DEK, a conserved non-histone chromatin protein, has recognized tumor-promoting properties, its overexpression being associated with poor prognosis in various cancer types. At the cellular level, DEK displays pleiotropic functions, influencing differentiation, apoptosis and stemness, but a characteristic oncogenic mechanism has remained elusive. Here, we report the identification of DEK bodies, focal assemblies of DEK that regularly occur at specific, yet unidentified, sites of heterochromatin replication exclusively in late S-phase. In these bodies, DEK localizes in direct proximity to active replisomes in agreement with a function in the early maturation of heterochromatin. A high-throughput siRNA screen, supported by mutational and biochemical analyses, identifies SUMO as one regulator of DEK body formation, linking DEK to the complex SUMO protein network that controls chromatin states and cell fate. This work combines and refines our previous data on DEK as a factor essential for heterochromatin integrity and facilitating replication under stress, and delineates an avenue of further study for unraveling the contribution of DEK to cancer development.</dcterms:abstract>
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