| Literature DB >> 27486244 |
Igor Cervenka1, Jana Valnohova1, Ondrej Bernatik2, Jakub Harnos1, Matej Radsetoulal1, Katerina Sedova3, Katerina Hanakova3, David Potesil3, Miroslava Sedlackova4, Alena Salasova5, Zachary Steinhart6, Stephane Angers6, Gunnar Schulte7, Ales Hampl4, Zbynek Zdrahal8, Vitezslav Bryja9.
Abstract
Dishevelled (DVL) is a key scaffolding protein and a branching point in Wnt signaling pathways. Here, we present conclusive evidence that DVL regulates the centrosomal cycle. We demonstrate that DVL dishevelled and axin (DIX) domain, but not DIX domain-mediated multimerization, is essential for DVL's centrosomal localization. DVL accumulates during the cell cycle and associates with NIMA-related kinase 2 (NEK2), which is able to phosphorylate DVL at a multitude of residues, as detected by a set of novel phospho-specific antibodies. This creates interfaces for efficient binding to CDK5 regulatory subunit-associated protein 2 (CDK5RAP2) and centrosomal Nek2-associated protein 1 (C-NAP1), two proteins of the centrosomal linker. Displacement of DVL from the centrosome and its release into the cytoplasm on NEK2 phosphorylation is coupled to the removal of linker proteins, an event necessary for centrosomal separation and proper formation of the mitotic spindle. Lack of DVL prevents NEK2-controlled dissolution of loose centrosomal linker and subsequent centrosomal separation. Increased DVL levels, in contrast, sequester centrosomal NEK2 and mimic monopolar spindle defects induced by a dominant negative version of this kinase. Our study thus uncovers molecular crosstalk between centrosome and Wnt signaling.Entities:
Keywords: Dishevelled; NEK2; Wnt signaling; centrosome; linker proteins
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Year: 2016 PMID: 27486244 PMCID: PMC4995965 DOI: 10.1073/pnas.1608783113
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205