Cdc25A activity is required for the metaphase II arrest in mouse oocytes | Zendy

Jeong Su Oh | Zendy; Andrej Šušor | Zendy; Karen Schindler | Zendy; Richard M. Schultz | Zendy; Marco Conti | Zendy

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Cdc25A activity is required for the metaphase II arrest in mouse oocytes

Author(s) -

Jeong Su Oh,

Andrej Šušor,

Karen Schindler,

Richard M. Schultz,

Marco Conti

Publication year - 2013

Publication title -

journal of cell science

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.384

H-Index - 278

eISSN - 1477-9137

pISSN - 0021-9533

DOI - 10.1242/jcs.115592

Subject(s) - biology , cyclin dependent kinase 1 , maturation promoting factor , metaphase , phosphorylation , cyclin b , cyclin b1 , microbiology and biotechnology , cyclin , biochemistry , cell cycle , chromosome , apoptosis , gene

Mammalian oocytes are arrested in metaphase of second meiosis (MII) until fertilization. This arrest is enforced by the cytostatic factor (CSF), which maintains the M-phase promoting factor (MPF) in a highly active state. Although the continuous synthesis and degradation of cyclin B to maintain the CSF-mediated MII arrest is well established, it is unknown whether cyclin-dependent kinase 1 (Cdk1) phosphorylations are involved in this arrest in mouse oocytes. Here, we show that a dynamic equilibrium of Cdk1 phosphorylation is required to maintain MII arrest. When the Cdc25A phosphatase is downregulated, mouse oocytes are released from MII arrest and MPF becomes inactivated. This inactivation occurs in the absence of cyclin B degradation and is dependent on Wee1B-mediated phosphorylation of Cdk1. Thus, our data demonstrate that Cdk1 activity is maintained during MII arrest not only by cyclin turnover but also by steady state phosphorylation.

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