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dc.contributor.authorSugimoto, Masataka
dc.contributor.authorMartin, Nicholas
dc.contributor.authorWilks, Deepti P
dc.contributor.authorTamai, Katsuyuki
dc.contributor.authorHuot, Thomas J G
dc.contributor.authorPantoja, Cristina
dc.contributor.authorOkumura, Ko
dc.contributor.authorSerrano, Manuel
dc.contributor.authorHara, Eiji
dc.date.accessioned2009-10-12T12:09:28Z
dc.date.available2009-10-12T12:09:28Z
dc.date.issued2002-11-21
dc.identifier.citationActivation of cyclin D1-kinase in murine fibroblasts lacking both p21(Cip1) and p27(Kip1). 2002, 21 (53):8067-74 Oncogeneen
dc.identifier.issn0950-9232
dc.identifier.pmid12444543
dc.identifier.doi10.1038/sj.onc.1206019
dc.identifier.urihttp://hdl.handle.net/10541/84057
dc.description.abstractDeregulation of D-type cyclin-dependent kinases (CDK4 and 6) is widely observed in various human cancers, illustrating their importance in cell cycle control. Like other cyclin-dependent kinases (CDKs), assembly with cyclins is the most critical step for activation of CDK4/6. As previously reported elsewhere, we observed that the level of cyclinD1-CDK4 complex and its associated kinase activity were significantly low in asynchronously proliferating mouse embryo fibroblasts lacking both p21(Cip1) and p27(Kip1) (p21/p27-null MEFs). These evidences imply that p21(Cip1) and p27(Kip1) CDK inhibitors are 'essential activators' of cyclin D-kinases. We, however, discovered here that both the assembly and activation of cyclin D1-CDK4 complex occur when quiescent p21/p27-null MEFs were stimulated to re-enter the cell cycle. This mitogen-induced cyclin D1-kinase activity was blocked by overexpression of p16(INK4a) and resulted in the inhibition of S phase entry in p21/p27-null MEFs. Furthermore, ectopic expression of p34(SEI-1), a mitogen-induced CDK4 binding protein, increased the levels of active cyclinD1-CDK4 complex in asynchronously proliferating p21/p27-null MEFs. Together, our results suggest that there are several independent ways to stimulate the assembly of cyclin D1-CDK4 kinases. Although p21(Cip1) and p27(Kip1) play a role in this process, our results demonstrate that additional mechanisms must occur in G0 to S phase transition.
dc.language.isoenen
dc.subjectFoetal Blooden
dc.subjectTumour Suppressor Proteinsen
dc.subject.meshAnimals
dc.subject.meshCattle
dc.subject.meshCell Cycle
dc.subject.meshCell Cycle Proteins
dc.subject.meshContact Inhibition
dc.subject.meshCulture Media
dc.subject.meshCulture Media, Serum-Free
dc.subject.meshCyclin-Dependent Kinase 4
dc.subject.meshCyclin-Dependent Kinase Inhibitor p21
dc.subject.meshCyclin-Dependent Kinase Inhibitor p27
dc.subject.meshCyclin-Dependent Kinases
dc.subject.meshCyclins
dc.subject.meshEmbryo, Mammalian
dc.subject.meshEnzyme Activation
dc.subject.meshFetal Blood
dc.subject.meshFibroblasts
dc.subject.meshG0 Phase
dc.subject.meshGene Targeting
dc.subject.meshGrowth Substances
dc.subject.meshHumans
dc.subject.meshMacromolecular Substances
dc.subject.meshMice
dc.subject.meshMitogens
dc.subject.meshNuclear Proteins
dc.subject.meshProto-Oncogene Proteins
dc.subject.meshS Phase
dc.subject.meshTrans-Activators
dc.subject.meshTumor Suppressor Proteins
dc.titleActivation of cyclin D1-kinase in murine fibroblasts lacking both p21(Cip1) and p27(Kip1).en
dc.typeArticleen
dc.contributor.departmentCancer Research UK, Paterson Institute for Cancer Research, Christie Hospital NHS Trust, Manchester M20 4BX, UK.en
dc.identifier.journalOncogeneen
html.description.abstractDeregulation of D-type cyclin-dependent kinases (CDK4 and 6) is widely observed in various human cancers, illustrating their importance in cell cycle control. Like other cyclin-dependent kinases (CDKs), assembly with cyclins is the most critical step for activation of CDK4/6. As previously reported elsewhere, we observed that the level of cyclinD1-CDK4 complex and its associated kinase activity were significantly low in asynchronously proliferating mouse embryo fibroblasts lacking both p21(Cip1) and p27(Kip1) (p21/p27-null MEFs). These evidences imply that p21(Cip1) and p27(Kip1) CDK inhibitors are 'essential activators' of cyclin D-kinases. We, however, discovered here that both the assembly and activation of cyclin D1-CDK4 complex occur when quiescent p21/p27-null MEFs were stimulated to re-enter the cell cycle. This mitogen-induced cyclin D1-kinase activity was blocked by overexpression of p16(INK4a) and resulted in the inhibition of S phase entry in p21/p27-null MEFs. Furthermore, ectopic expression of p34(SEI-1), a mitogen-induced CDK4 binding protein, increased the levels of active cyclinD1-CDK4 complex in asynchronously proliferating p21/p27-null MEFs. Together, our results suggest that there are several independent ways to stimulate the assembly of cyclin D1-CDK4 kinases. Although p21(Cip1) and p27(Kip1) play a role in this process, our results demonstrate that additional mechanisms must occur in G0 to S phase transition.


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