SET8 is degraded via PCNA-coupled CRL4(CDT2) ubiquitylation in S phase and after UV irradiation |
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Authors: | Jørgensen Stine Eskildsen Morten Fugger Kasper Hansen Lisbeth Larsen Marie Sofie Yoo Kousholt Arne Nedergaard Syljuåsen Randi G Trelle Morten Beck Jensen Ole Nørregaard Helin Kristian Sørensen Claus Storgaard |
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Affiliation: | 1Biotech Research and Innovation Centre, and 2Centre for Epigenetics, University of Copenhagen, 2200 Copenhagen, Denmark;3Centre for Epigenetics, and 4Department of Biochemistry and Molecular Biology, University of Southern Denmark, 5230 Odense, Denmark;5Department of Radiation Biology, Institute for Cancer Research, The Norwegian Radium Hospital, 0310 Oslo, Norway |
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Abstract: | The eukaryotic cell cycle is regulated by multiple ubiquitin-mediated events, such as the timely destruction of cyclins and replication licensing factors. The histone H4 methyltransferase SET8 (Pr-Set7) is required for chromosome compaction in mitosis and for maintenance of genome integrity. In this study, we show that SET8 is targeted for degradation during S phase by the CRL4(CDT2) ubiquitin ligase in a proliferating cell nuclear antigen (PCNA)-dependent manner. SET8 degradation requires a conserved degron responsible for its interaction with PCNA and recruitment to chromatin where ubiquitylation occurs. Efficient degradation of SET8 at the onset of S phase is required for the regulation of chromatin compaction status and cell cycle progression. Moreover, the turnover of SET8 is accelerated after ultraviolet irradiation dependent on the CRL4(CDT2) ubiquitin ligase and PCNA. Removal of SET8 supports the modulation of chromatin structure after DNA damage. These results demonstrate a novel regulatory mechanism, linking for the first time the ubiquitin-proteasome system with rapid degradation of a histone methyltransferase to control cell proliferation. |
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