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Literature DB >> 11553706

Cyclin B/cdc2 induces c-Mos stability by direct phosphorylation in Xenopus oocytes.

A Castro¹, M Peter, L Magnaghi-Jaulin, S Vigneron, S Galas, T Lorca, J C Labbé.

Abstract

The c-Mos proto-oncogene product plays an essential role during meiotic divisions in vertebrate eggs. In Xenopus, it is required for progression of oocyte maturation and meiotic arrest of unfertilized eggs. Its degradation after fertilization is essential to early embryogenesis. In this study we investigated the mechanisms involved in c-Mos degradation. We present in vivo evidence for ubiquitin-dependent degradation of c-Mos in activated eggs. We found that c-Mos degradation is not directly dependent on the anaphase-promoting factor activator Fizzy/cdc20 but requires cyclin degradation. We demonstrate that cyclin B/cdc2 controls in vivo c-Mos phosphorylation and stabilization. Moreover, we show that cyclin B/cdc2 is capable of directly phosphorylating c-Mos in vitro, inducing a similar mobility shift to the one observed in vivo. Tryptic phosphopeptide analysis revealed a practically identical in vivo and in vitro phosphopeptide map and allowed identification of serine-3 as the largely preferential phosphorylation site as previously described (Freeman et al., 1992). Altogether, these results demonstrate that, in vivo, stability of c-Mos is directly regulated by cyclin B/cdc2 kinase activity.

Entities: Chemical Gene Species

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Year: 2001 PMID： 11553706 PMCID： PMC59702 DOI： 10.1091/mbc.12.9.2660

Source DB: PubMed Journal: Mol Biol Cell ISSN： 1059-1524 Impact factor: 4.138

49 in total

1. Residual Cdc2 activity remaining at meiosis I exit is essential for meiotic M-M transition in Xenopus oocyte extracts.

Authors: M Iwabuchi; K Ohsumi; T M Yamamoto; W Sawada; T Kishimoto
Journal: EMBO J Date: 2000-09-01 Impact factor: 11.598

2. Positive feedback between MAP kinase and Mos during Xenopus oocyte maturation.

Authors: W T Matten; T D Copeland; N G Ahn; G F Vande Woude
Journal: Dev Biol Date: 1996-11-01 Impact factor: 3.582

3. Newly assembled cyclin B-cdc2 kinase is required to suppress DNA replication between meiosis I and meiosis II in starfish oocytes.

Authors: A Picard; S Galas; G Peaucellier; M Dorée
Journal: EMBO J Date: 1996-07-15 Impact factor: 11.598

Review 4. What does Mos do in oocytes and somatic cells?

Authors: N Sagata
Journal: Bioessays Date: 1997-01 Impact factor: 4.345

5. The critical role of the MAP kinase pathway in meiosis II in Xenopus oocytes is mediated by p90(Rsk).

Authors: S D Gross; M S Schwab; F E Taieb; A L Lewellyn; Y W Qian; J L Maller
Journal: Curr Biol Date: 2000-04-20 Impact factor: 10.834

6. Inhibition of v-Mos kinase activity by protein kinase A.

Authors: Y Yang; C H Herrmann; R B Arlinghaus; B Singh
Journal: Mol Cell Biol Date: 1996-03 Impact factor: 4.272

7. The protein kinase p90 rsk as an essential mediator of cytostatic factor activity.

Authors: R R Bhatt; J E Ferrell
Journal: Science Date: 1999-11-12 Impact factor: 47.728

8. Mos proto-oncogene function during oocyte maturation in Xenopus.

Authors: L M Roy; O Haccard; T Izumi; B G Lattes; A L Lewellyn; J L Maller
Journal: Oncogene Date: 1996-05-16 Impact factor: 9.867

9. Degradation of Mos by the N-terminal proline (Pro2)-dependent ubiquitin pathway on fertilization of Xenopus eggs: possible significance of natural selection for Pro2 in Mos.

Authors: M Nishizawa; N Furuno; K Okazaki; H Tanaka; Y Ogawa; N Sagata
Journal: EMBO J Date: 1993-10 Impact factor: 11.598

10. MAP kinase does not inactivate, but rather prevents the cyclin degradation pathway from being turned on in Xenopus egg extracts.

Authors: A Abrieu; T Lorca; J C Labbé; N Morin; S Keyse; M Dorée
Journal: J Cell Sci Date: 1996-01 Impact factor: 5.285

24 in total

Cyclin B/cdc2 induces c-Mos stability by direct phosphorylation in Xenopus oocytes.

1. Residual Cdc2 activity remaining at meiosis I exit is essential for meiotic M-M transition in Xenopus oocyte extracts.

2. Positive feedback between MAP kinase and Mos during Xenopus oocyte maturation.

3. Newly assembled cyclin B-cdc2 kinase is required to suppress DNA replication between meiosis I and meiosis II in starfish oocytes.

Review 4. What does Mos do in oocytes and somatic cells?

5. The critical role of the MAP kinase pathway in meiosis II in Xenopus oocytes is mediated by p90(Rsk).

6. Inhibition of v-Mos kinase activity by protein kinase A.

7. The protein kinase p90 rsk as an essential mediator of cytostatic factor activity.

8. Mos proto-oncogene function during oocyte maturation in Xenopus.

9. Degradation of Mos by the N-terminal proline (Pro2)-dependent ubiquitin pathway on fertilization of Xenopus eggs: possible significance of natural selection for Pro2 in Mos.

10. MAP kinase does not inactivate, but rather prevents the cyclin degradation pathway from being turned on in Xenopus egg extracts.

1. A novel regulatory element determines the timing of Mos mRNA translation during Xenopus oocyte maturation.

2. APC/Fizzy-Related targets Aurora-A kinase for proteolysis.

3. Xkid is degraded in a D-box, KEN-box, and A-box-independent pathway.

4. The D-Box-activating domain (DAD) is a new proteolysis signal that stimulates the silent D-Box sequence of Aurora-A.

5. Autoregulation of Musashi1 mRNA translation during Xenopus oocyte maturation.

6. Mechanistic studies of the mitotic activation of Mos.

7. Redundant pathways for Cdc2 activation in Xenopus oocyte: either cyclin B or Mos synthesis.

8. Characterization of the mechanisms controlling Greatwall activity.

9. Paxillin and steroid signaling: from frog to human.

10. Release from meiotic arrest in ascidian eggs requires the activity of two phosphatases but not CaMKII.