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The centrosomal component CEP161 of Dictyostelium discoideum interacts with the Hippo signaling pathway.


ABSTRACT: CEP161 is a novel component of the Dictyostelium discoideum centrosome which was identified as binding partner of the pericentriolar component CP250. Here we show that the amino acids 1-763 of the 1381 amino acids CEP161 are sufficient for CP250 binding, centrosomal targeting and centrosome association. Analysis of AX2 cells over-expressing truncated and full length CEP161 proteins revealed defects in growth and development. By immunoprecipitation experiments we identified the Hippo related kinase SvkA (Hrk-svk) as binding partner for CEP161. Both proteins colocalize at the centrosome. In in vitro kinase assays the N-terminal domain of CEP161 (residues 1-763) inhibited the kinase activity of Hrk-svk. A comparison of D. discoideum Hippo kinase mutants with mutants overexpressing CEP161 polypeptides revealed similar defects. We propose that the centrosomal component CEP161 is a novel player in the Hippo signaling pathway and affects various cellular properties through this interaction.

SUBMITTER: Sukumaran SK 

PROVIDER: S-EPMC4614953 | biostudies-other | 2015

REPOSITORIES: biostudies-other

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The centrosomal component CEP161 of Dictyostelium discoideum interacts with the Hippo signaling pathway.

Sukumaran Salil K SK   Blau-Wasser Rosemarie R   Rohlfs Meino M   Gallinger Christoph C   Schleicher Michael M   Noegel Angelika A AA  

Cell cycle (Georgetown, Tex.) 20150101 7


CEP161 is a novel component of the Dictyostelium discoideum centrosome which was identified as binding partner of the pericentriolar component CP250. Here we show that the amino acids 1-763 of the 1381 amino acids CEP161 are sufficient for CP250 binding, centrosomal targeting and centrosome association. Analysis of AX2 cells over-expressing truncated and full length CEP161 proteins revealed defects in growth and development. By immunoprecipitation experiments we identified the Hippo related kina  ...[more]

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