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Glycogen synthase kinase 3 ? activity is required for hBora/Aurora A-mediated mitotic entry.


ABSTRACT: The synthesis and degradation of hBora is important for the regulation of mitotic entry and exist. In G 2 phase, hBora can complex with Aurora A to activate Plk1 and control mitotic entry. However, whether the post-translational modification of hBora is relevant to the mitotic entry still unclear. Here, we used the LC-MS/MS phosphopeptide mapping assay to identify 13 in vivo hBora phosphorylation sites and characterized that GSK3? can interact with hBora and phosphorylate hBora at Ser274 and Ser278. Pharmacological inhibitors of GSK3? reduced the retarded migrating band of hBora in cells and diminished the phosphorylation of hBora by in vitro kinase assay. Moreover, as well as in GSK3? activity-inhibited cells, specific knockdown of GSK3? by shRNA and S274A/S278 hBora mutant-expressing cells also exhibited the reduced Plk1 activation and a delay in mitotic entry. It suggests that GSK3? activity is required for hBora-mediated mitotic entry through Ser274 and Ser278 phosphorylation.

SUBMITTER: Lee YC 

PROVIDER: S-EPMC3637354 | biostudies-literature | 2013 Mar

REPOSITORIES: biostudies-literature

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Glycogen synthase kinase 3 β activity is required for hBora/Aurora A-mediated mitotic entry.

Lee Yu-Cheng YC   Liao Po-Chi PC   Liou Yih-Cherng YC   Hsiao Michael M   Huang Chi-Ying CY   Lu Pei-Jung PJ  

Cell cycle (Georgetown, Tex.) 20130226 6


The synthesis and degradation of hBora is important for the regulation of mitotic entry and exist. In G 2 phase, hBora can complex with Aurora A to activate Plk1 and control mitotic entry. However, whether the post-translational modification of hBora is relevant to the mitotic entry still unclear. Here, we used the LC-MS/MS phosphopeptide mapping assay to identify 13 in vivo hBora phosphorylation sites and characterized that GSK3β can interact with hBora and phosphorylate hBora at Ser274 and Ser  ...[more]

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