Cdc2-cyclin E complexes regulate the G1/S phase transition
- PMID: 16007079
- DOI: 10.1038/ncb1284
Cdc2-cyclin E complexes regulate the G1/S phase transition
Abstract
The cyclin-dependent kinase inhibitor p27(Kip1) is known as a negative regulator of cell-cycle progression and as a tumour suppressor. Cdk2 is the main target of p27 (refs 2, 3) and therefore we hypothesized that loss of Cdk2 activity should modify the p27(-/-) mouse phenotype. Here, we show that although p27(-/-) Cdk2(-/-) mice developed ovary tumours and tumours in the anterior lobe of the pituitary, we failed to detect any functional complementation in p27(-/-) Cdk2(-/-) double-knockout mice, indicating a parallel pathway regulated by p27. We observed elevated levels of S phase and mitosis in tissues of p27(-/-) Cdk2(-/-) mice concomitantly with elevated Cdc2 activity in p27(-/-) Cdk2(-/-) extracts. p27 binds to Cdc2, cyclin B1, cyclin A2, or suc1 complexes in wild-type and Cdk2(-/-) extracts. In addition, cyclin E binds to and activates Cdc2. Our in vivo results provide strong evidence that Cdc2 may compensate the loss of Cdk2 function.
Comment in
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Cdk1: the dominant sibling of Cdk2.Nat Cell Biol. 2005 Aug;7(8):779-81. doi: 10.1038/ncb0805-779. Nat Cell Biol. 2005. PMID: 16056272 No abstract available.
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