4.7 Article

CDC6 regulates both G2/M transition and metaphase-to-anaphase transition during the first meiosis of mouse oocytes

期刊

JOURNAL OF CELLULAR PHYSIOLOGY
卷 235, 期 7-8, 页码 5541-5554

出版社

WILEY
DOI: 10.1002/jcp.29469

关键词

CDC6; germinal vesicle breakdown; meiosis; oocyte; spindle

资金

  1. Project for Medical Discipline Advancement of Health and Family Planning commission of Shenzhen Municipality [SZXJ2017003]
  2. National Natural Science Foundation of China [31530049]
  3. Research Team of Female Reproductive Health and Fertility Preservation [SZSM201612065]
  4. Exploration of New method of Noninvasive Fertility Evaluation and Establishment of National Standard [2018YFC1002104]
  5. Natural Science Foundation of Guangdong Province [2018A030310673]

向作者/读者索取更多资源

Cell division cycle protein, CDC6, is essential for the initiation of DNA replication. CDC6 was recently shown to inhibit the microtubule-organizing activity of the centrosome. Here, we show that CDC6 is localized to the spindle from pro-metaphase I (MI) to MII stages of oocytes, and it plays important roles at two critical steps of oocyte meiotic maturation. CDC6 depletion facilitated the G2/M transition (germinal vesicle breakdown [GVBD]) through regulation of Cdh1 and cyclin B1 expression and CDK1 (CDC2) phosphorylation in a GVBD-inhibiting culture system containing milrinone. Furthermore, GVBD was significantly decreased after knockdown of cyclin B1 in CDC6-depleted oocytes, indicating that the effect of CDC6 loss on GVBD stimulation was mediated, at least in part, by raising cyclin B1. Knockdown of CDC6 also caused abnormal localization of gamma-tubulin, resulting in defective spindles, misaligned chromosomes, cyclin B1 accumulation, and spindle assembly checkpoint (SAC) activation, leading to significant pro-MI/MI arrest and PB1 extrusion failure. These phenotypes were also confirmed by time-lapse live cell imaging analysis. The results indicate that CDC6 is indispensable for maintaining G2 arrest of meiosis and functions in G2/M checkpoint regulation in mouse oocytes. Moreover, CDC6 is also a key player regulating meiotic spindle assembly and metaphase-to-anaphase transition in meiotic oocytes.

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