| Literature DB >> 26766443 |
Ksenia Krupina1, Charlotte Kleiss1, Thibaud Metzger1, Sadek Fournane1, Stephane Schmucker1, Kay Hofmann2, Benoit Fischer1, Nicodeme Paul3, Iain Malcolm Porter4, Wolfgang Raffelsberger5, Olivier Poch6, Jason Reese Swedlow4, Laurent Brino1, Izabela Sumara7.
Abstract
Mitosis ensures equal segregation of the genome and is controlled by a variety of ubiquitylation signals on substrate proteins. However, it remains unexplored how the versatile ubiquitin code is read out during mitotic progression. Here, we identify the ubiquitin receptor protein UBASH3B as an important regulator of mitosis. UBASH3B interacts with ubiquitylated Aurora B, one of the main kinases regulating chromosome segregation, and controls its subcellular localization but not protein levels. UBASH3B is a limiting factor in this pathway and is sufficient to localize Aurora B to microtubules prior to anaphase. Importantly, targeting Aurora B to microtubules by UBASH3B is necessary for the timing and fidelity of chromosome segregation in human cells. Our findings uncover an important mechanism defining how ubiquitin attachment to a substrate protein is decoded during mitosis.Entities:
Keywords: Aurora B; UBASH3B; chromosome segregation; mitosis; ubiquitin; ubiquitin receptor
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Year: 2016 PMID: 26766443 PMCID: PMC5400057 DOI: 10.1016/j.devcel.2015.12.017
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270