| Literature DB >> 32772043 |
Mara Esposito1, H Begum Akman2, Philippe Giron1,3, M Angeles Ceregido1,4, Rogier Schepers1,5, Luis C Ramos Paez1,6, Esther La Monaca1,7, Jacques De Greve3, Olivier Coux8, Carl De Trez9, Catherine Lindon2, Gustavo J Gutierrez10,11.
Abstract
Aurora B kinase plays essential roles in mitosis. Its protein levels increase before the onset of mitosis and sharply decrease during mitosis exit. The latter decrease is due to a balance between the actions of the E3 ubiquitin ligase anaphase-promoting complex or cyclosome (activated by the Cdh1 adapter), and the deubiquitinating enzyme USP35. Aurora B also executes important functions in interphase. Abnormal modulation of Aurora B in interphase leads to cell cycle defects often linked to aberrant chromosomal condensation and segregation. Very little is however known about how Aurora B levels are regulated in interphase. Here we found that USP13-associates with and stabilizes Aurora B in cells, especially before their entry into mitosis. In order for USP13 to exert its stabilizing effect on Aurora B, their association is promoted by the Aurora B-mediated phosphorylation of USP13 at Serine 114. We also present evidence that USP13 instigates Aurora B deubiquitination and/or protect it from degradation in a non-catalytic manner. In addition, we report that genetic or chemical modulation of the cellular levels/activity of USP13 affects unperturbed cell-cycle progression. Overall our study unveils the molecular and cellular connections of the USP13-Aurora B axis, which potentially participates in the rewiring of the cell cycle happening in cancer cells.Entities:
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Year: 2020 PMID: 32772043 DOI: 10.1038/s41388-020-01396-8
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867