Literature DB >> 11401401

Meiotic maturation of the mouse oocyte requires an equilibrium between cyclin B synthesis and degradation.

E Ledan1, Z Polanski, M E Terret, B Maro.   

Abstract

Among the proteins whose synthesis and/or degradation is necessary for a proper progression through meiotic maturation, cyclin B appears to be one of the most important. Here, we attempted to modulate the level of cyclin B1 and B2 synthesis during meiotic maturation of the mouse oocyte. We used cyclin B1 or B2 mRNAs with poly(A) tails of different sizes and cyclin B1 or B2 antisense RNAs. Oocytes microinjected with cyclin B1 mRNA showed two phenotypes: most were blocked in MI, while the others extruded the first polar body in advance when compared to controls. Moreover, these effects were correlated with the length of the poly(A) tail. Thus it seems that the rate of cyclin B1 translation controls the timing of the first meiotic M phase and the transition to anaphase I. Moreover, overexpression of cyclin B1 or B2 was able to bypass the dbcAMP-induced germinal vesicle block, but only the cyclin B1 mRNA-microinjected oocytes did not extrude their first polar body. Oocytes injected with the cyclin B1 antisense progressed through the first meiotic M phase but extruded the first polar body in advance and were unable to enter metaphase II. This suggested that inhibition of cyclin B1 synthesis only took place at the end of the first meiotic M phase, most likely because the cyclin B1 mRNA was protected. The injection of cyclin B2 antisense RNA had no effect. The life observation of the synthesis and degradation of a cyclin B1-GFP chimera during meiotic maturation of the mouse oocyte demonstrated that degradation can only occur during a given period of time once it has started. Taken together, our data demonstrate that the rates of cyclin B synthesis and degradation determine the timing of the major events taking place during meiotic maturation of the mouse oocyte. Copyright 2001 Academic Press.

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Year:  2001        PMID: 11401401     DOI: 10.1006/dbio.2001.0188

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  40 in total

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2.  RFPL4 interacts with oocyte proteins of the ubiquitin-proteasome degradation pathway.

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Review 6.  Modulation of cell cycle control during oocyte-to-embryo transitions.

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7.  PKCβ1 regulates meiotic cell cycle in mouse oocyte.

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Review 8.  Principles and mechanisms of asymmetric cell division.

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9.  Biased inheritance of mitochondria during asymmetric cell division in the mouse oocyte.

Authors:  Caroline M Dalton; John Carroll
Journal:  J Cell Sci       Date:  2013-05-09       Impact factor: 5.285

10.  The cyclin-A CYCA1;2/TAM is required for the meiosis I to meiosis II transition and cooperates with OSD1 for the prophase to first meiotic division transition.

Authors:  Isabelle d'Erfurth; Laurence Cromer; Sylvie Jolivet; Chloé Girard; Christine Horlow; Yujin Sun; Jennifer P C To; Luke E Berchowitz; Gregory P Copenhaver; Raphael Mercier
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