Literature DB >> 9429304

Stability of cyclin B protein during meiotic maturation and the first mitotic cell division in mouse oocytes.

N J Winston1.   

Abstract

This report examines in detail the metabolism of the cyclin protein B1 during meiotic maturation and following the activation of mature mouse oocytes using immunoprecipitation of the radiolabelled protein. The net synthesis of cyclin B increases progressively during meiotic maturation, reaching its maximum levels at least 1 h before oocytes exit into metaphase of meiosis II (MII). This increase correlates with the rise in cdc2 kinase activity reported previously and suggests an association between the length of the first meiotic M phase (MI) and the net synthesis of cyclin B, that seems to regulate the time required for the cdc2 kinase to reach its maximum activity. Moreover, no marked degradation of cyclin B was observed before the MI to MII transition and that which occurs does so independently of the presence of microtubules, which are essential for cyclin degradation during metaphase II arrest and exit of oocytes into interphase of the first mitotic cell cycle. Cyclin B is degraded rapidly during the transitions MI to MII, MII to the first mitotic interphase and MII to an abortive third metaphase state (MIII). However, whilst its degradation was incomplete during the MI to MII transition, virtually no cyclin B protein was detected following both the MII to interphase and MII to MIII transitions. Thus, the decision of oocytes to exit into MIII, or interphase is not controlled at the level of cyclin B degradation. Lastly, in aging, non-activated oocytes, the net synthesis of cyclin B declines. Whereas, in activated eggs cultured in parallel although the rate of net synthesis declines initially, it is effectively 'rescued' being two-fold greater than in non-activated oocytes of an equivalent age. This gradual fall in the net synthesis of cyclin B observed in aging oocytes may contribute to the increasing ease with which they become activated, compared to recently ovulated oocytes.

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Year:  1997        PMID: 9429304

Source DB:  PubMed          Journal:  Biol Cell        ISSN: 0248-4900            Impact factor:   4.458


  8 in total

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Review 2.  Oocyte maturation failure: a syndrome of bad eggs.

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Journal:  Nature       Date:  2014-04-28       Impact factor: 49.962

Review 4.  Translational activation of maternally derived mRNAs in oocytes and early embryos and the role of embryonic poly(A) binding protein (EPAB).

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6.  Increased CDK1 activity determines the timing of kinetochore-microtubule attachments in meiosis I.

Authors:  Olga Davydenko; Richard M Schultz; Michael A Lampson
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7.  Mysteries in embryonic development: How can errors arise so frequently at the beginning of mammalian life?

Authors:  Isabell Schneider; Jan Ellenberg
Journal:  PLoS Biol       Date:  2019-03-06       Impact factor: 8.029

8.  Developmental and Degenerative Characterization of Porcine Parthenogenetic Fetuses during Early Pregnancy.

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Journal:  Animals (Basel)       Date:  2020-04-04       Impact factor: 2.752

  8 in total

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