The APC/C activator FZR1 coordinates the timing of meiotic resumption during prophase I arrest in mammalian oocytes

Holt, Janet E.; Tran, Suzanne My-Trinh; Stewart, Jessica L.; Minahan, Kyra; García-Higuera, Irene; Moreno, Sergio; Jones, Kevin

doi:10.1242/dev.059022

Cited by 57 publications

(71 citation statements)

References 75 publications

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“…Reduction of activity of ETC-1 and APC/C also caused the premature NEBD phenotype with low-penetrance during prophase I. In mammalian oocytes, APC/C activity is required to maintain low cyclin B1 levels during prophase I arrest (Reis et al, 2007;Holt et al, 2011). CYB-1-dependent phosphorylation of the nuclear pore component NPP-12 (Gp210) is required for timely NEBD during mitosis (Galy et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

HECT-E3 ligase ETC-1 regulates securin and cyclin B1 cytoplasmic abundance to promote timely anaphase during meiosis inC. elegans

et al. 2013

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SUMMARYThe anaphase inhibitor securin plays a crucial role in regulating the timing of sister chromatid separation during mitosis. When sister chromatid pairs become bioriented, the E3 ligase anaphase promoting complex/cyclosome (APC/C) ubiquitylates securin for proteolysis, triggering sister chromatid separation. Securin is also implicated in regulating meiotic progression. Securin protein levels change sharply during cell cycle progression, enabling its timely action. To understand the mechanism underlying the tightly regulated dynamics of securin, we analyzed the subcellular localization of the securin IFY-1 during C. elegans development. IFY-1 was highly expressed in the cytoplasm of germ cells. The cytoplasmic level of IFY-1 declined immediately following meiosis I division and remained low during meiosis II and following mitoses. We identified a C. elegans homolog of another type of E3 ligase, UBE3C, designated ETC-1, as a regulator of the cytoplasmic IFY-1 level. RNAi-mediated depletion of ETC-1 stabilized IFY-1 and CYB-1 (cyclin B1) in post-meiosis I embryos. ETC-1 knockdown in a reduced APC function background caused an embryonic lethal phenotype. In vitro, ETC-1 ubiquitylates IFY-1 and CYB-1 in the presence of the E2 enzyme UBC-18, which functions in pharyngeal development. Genetic analysis revealed that UBC-18 plays a distinct role together with ETC-1 in regulating the cytoplasmic level of IFY-1 during meiosis. Our study reports a novel mechanism, mediated by ETC-1, that co-operates with APC/C to maintain the meiotic arrest required for proper cell cycle timing during reproduction.

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Section: Discussionmentioning

confidence: 99%

HECT-E3 ligase ETC-1 regulates securin and cyclin B1 cytoplasmic abundance to promote timely anaphase during meiosis inC. elegans

et al. 2013

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“…Significantly, even within the inhibitory cAMP-rich follicular environment within the ovary, Fzr1 D/D oocytes exhibited an increased tendency to undergo GVBD that was related to elevated cyclin B1 levels. Importantly, in Fzr1 D/D oocytes, there was no change in the levels of Cdc25B, a potential APC/C Cdh1 substrate (Holt et al 2011), altogether underlining the importance of the APC/ C-cyclin B1 pathway for regulating G2/prophase arrest independent of Cdk1 phosphorylation status. Interestingly, even though many aspects of follicular physiology remained intact in Fzr1 D/D mutant mice, there was nevertheless a 35-40% reduction in the numbers of cumulus-enclosed oocytes (Holt et al 2011), suggesting that defects in oocyte-centred control brought about through APC/C de-regulation were detrimental to overall follicular health and integrity.…”

Section: Cdh1mentioning

confidence: 93%

“…It was found that such Cdh1-depleted oocytes exhibited an increased susceptibility to undergoing GVBD even under conditions in which cAMP levels were chemically sustained using the phosphodiesterase inhibitor, milrinone. More recently, this mechanism has R62 H Homer been shown to be physiologically relevant for sustaining the reservoir of G2/prophase-arrested oocytes using an in vivo mouse model in which Fzr1 was specifically deleted from growing and mature oocytes using Cre-LoxP technology (Fzr1 D/D mice; Holt et al 2011). Significantly, even within the inhibitory cAMP-rich follicular environment within the ovary, Fzr1 D/D oocytes exhibited an increased tendency to undergo GVBD that was related to elevated cyclin B1 levels.…”

Section: Cdh1mentioning

confidence: 99%

The APC/C in female mammalian meiosis I

Homer¹

2013

Reproduction

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The anaphase-promoting complex or cyclosome (APC/C) orchestrates a meticulously controlled sequence of proteolytic events critical for proper cell cycle progression, the details of which have been most extensively elucidated during mitosis. It has become apparent, however, that the APC/C, particularly when acting in concert with its Cdh1 co-activator (APC/C Cdh1 ), executes a staggeringly diverse repertoire of functions that extend its remit well outside the bounds of mitosis. Findings over the past decade have not only earmarked mammalian oocyte maturation as one such case in point but have also begun to reveal a complex pattern of APC/C regulation that underpins many of the oocyte's unique developmental attributes. This review will encompass the latest findings pertinent to the APC/C, especially APC/C Cdh1 , in mammalian oocytes and how its activity and substrates shape the stop-start tempo of female mammalian first meiotic division and the challenging requirement for assembling spindles in the absence of centrosomes.Reproduction (2013) 146 R61-R71

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“…Oocytes were handled in M2 media containing 2.5 µM milrinone (Sigma-Aldrich) under mineral oil at 37 °C, and maturation was stimulated by milrinone washout, timed relative to extrusion of the first polar body. 70 Microinjections were performed on the heated stage of a Nikon TE300 inverted microscope as previously described.…”

Section: Methodsmentioning

confidence: 99%

Reduced ability to recover from spindle disruption and loss of kinetochore spindle assembly checkpoint proteins in oocytes from aged mice

et al. 2014

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The APC/C activator FZR1 coordinates the timing of meiotic resumption during prophase I arrest in mammalian oocytes

Cited by 57 publications

References 75 publications

HECT-E3 ligase ETC-1 regulates securin and cyclin B1 cytoplasmic abundance to promote timely anaphase during meiosis inC. elegans

HECT-E3 ligase ETC-1 regulates securin and cyclin B1 cytoplasmic abundance to promote timely anaphase during meiosis inC. elegans

The APC/C in female mammalian meiosis I

Reduced ability to recover from spindle disruption and loss of kinetochore spindle assembly checkpoint proteins in oocytes from aged mice

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