| Literature DB >> 31640856 |
Tie-Gang Meng1, Wen-Long Lei2, Jian Li3, Feng Wang1, Zheng-Hui Zhao2, Ang Li3, Zhen-Bo Wang2, Qing-Yuan Sun2, Xiang-Hong Ou4.
Abstract
Before fertilization, ovulated mammalian oocytes are arrested at the metaphase of second meiosis (MII), which is maintained by the so-called cytostatic factor (CSF). It is well known that the continuous synthesis and accumulation of cyclin B is critical for maintaining the CSF-mediated MII arrest. Recent studies by us and others have shown that Ccnb3 is required for the metaphase-to-anaphase transition during the first meiosis of mouse oocytes, but whether Ccnb3 plays a role in MII arrest and exit remains unknown. Here, we showed that the protein level of Ccnb3 gradually decreased during oocyte meiotic maturation, and exogenous expression of Ccnb3 led to release of MII arrest, degradation of securin, separation of sister chromatids, extrusion of the second polar body (PB2), and finally entry into interphase. These phenotypes could be rescued by inhibition of Wee1B or CDK2. Our results indicate that Ccnb3 plays a critical regulatory role in MII arrest and exit in mouse oocytes.Entities:
Keywords: Ccnb3; MII arrest; MII exit; Oocyte
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Year: 2019 PMID: 31640856 DOI: 10.1016/j.bbrc.2019.10.124
Source DB: PubMed Journal: Biochem Biophys Res Commun ISSN: 0006-291X Impact factor: 3.575