Access
To read this story in full you will need to login or make a payment (see right).
Letter
Nature 449, 336-340 (20 September 2007) | doi:10.1038/nature06121; Received 4 May 2007; Accepted 26 July 2007
Open Innovation Challenges
-
Protect Enzyme from In Planta Degradation
A proposal for stable expression of an enzyme in corn seed is desired.
-
Efficient Chromosome Doubling: Plant Cell Division
The Seeker is looking for an efficient chromosome doubling method in plants and in particular, metho...
- More Challenges
- Powered by:
nature jobs
Behavioural Pharmacologist
- Eisai London Research Laboratories Ltd
- Hatfield, United Kingdom
Assistant or Associate Professor
- Texas Tech University Health Sciences Center
- Lubbock, TX United States
Calcineurin is required to release Xenopus egg extracts from meiotic M phase
- Cancer Research UK, London Research Institute, Clare Hall Laboratories, South Mimms, Hertfordshire EN6 3LD, UK
Correspondence to: Tim Hunt1 Correspondence and requests for materials should be addressed to T.H. (Email: tim.hunt@cancer.org.uk).
Abstract
Fertilization induces a transient increase in cytoplasmic Ca2+ concentration in animal eggs that releases them from cell cycle arrest in the second meiotic metaphase1. In frog eggs, Ca2+ activates Ca2+/calmodulin-activated kinase, which inactivates cytostatic factor2, 3, 4, 5, allowing the anaphase-promoting factor to turn on and ubiquitinate cyclins and securin, which returns the cell cycle to interphase6. Here we show that the calcium-activated protein phosphatase calcineurin7 is also important in this process. Calcineurin is transiently activated after adding Ca2+ to egg extracts, and inhibitors of calcineurin such as cyclosporin A (ref. 8) delay the destruction of cyclins, the global dephosphorylation of M-phase-specific phosphoproteins and the re-formation of a fully functional nuclear envelope. We found that a second wave of phosphatase activity directed at mitotic phosphoproteins appears after the spike of calcineurin activity. This activity disappeared the next time the extract entered M phase and reappeared at the end of mitosis. We surmise that inhibition of this second phosphatase activity is important in allowing cells to enter mitosis, and, conversely, that its activation is required for a timely return to interphase. Calcineurin is required to break the deep cell cycle arrest imposed by the Mos-MAP (mitogen-activated protein) kinase pathway4, 5, 9, and we show that Fizzy/Cdc20, a key regulator of the anaphase-promoting factor6, is an excellent substrate for this phosphatase.
- Cancer Research UK, London Research Institute, Clare Hall Laboratories, South Mimms, Hertfordshire EN6 3LD, UK
Correspondence to: Tim Hunt1 Correspondence and requests for materials should be addressed to T.H. (Email: tim.hunt@cancer.org.uk).
To read this story in full you will need to login or make a payment (see right).
MORE ARTICLES LIKE THIS
These links to content published by NPG are automatically generated.
NEWS AND VIEWS
Fertilization Calcium's double punchNature News and Views (20 Sep 2007)
Conspiracy to disarm APC in interphaseNature Cell Biology News and Views (01 May 2002)
See all 7 matches for News And ViewsRESEARCH
A GTP-binding adapter protein couples TRAIL receptors to apoptosis-inducing proteinsNature Immunology Article (01 Jun 2001)
PP1-mediated dephosphorylation of phosphoproteins at mitotic exit is controlled by inhibitor-1 and PP1 phosphorylationNature Cell Biology Letter (01 May 2009)
See all 56 matches for Research