Brush GS, et al. (2012)

Reference: Brush GS, et al. (2012) Yeast IME2 functions early in meiosis upstream of cell cycle-regulated SBF and MBF targets. PLoS One 7(2):e31575

Reference Help

Abstract

Background: In Saccharomyces cerevisiae, the G1 cyclin/cyclin-dependent kinase (CDK) complexes Cln1,-2,-3/Cdk1 promote S phase entry during the mitotic cell cycle but do not function during meiosis. It has been proposed that the meiosis-specific protein kinase Ime2, which is required for normal timing of pre-meiotic DNA replication, is equivalent to Cln1,-2/Cdk1. These two CDK complexes directly catalyze phosphorylation of the B-type cyclin/CDK inhibitor Sic1 during the cell cycle to enable its destruction. As a result, Clb5,-6/Cdk1 become activated and facilitate initiation of DNA replication. While Ime2 is required for Sic1 destruction during meiosis, evidence now suggests that Ime2 does not directly catalyze Sic1 phosphorylation to target it for destabilization as Cln1,-2/Cdk1 do during the cell cycle.

Methodology/principal findings: We demonstrated that Sic1 is eventually degraded in meiotic cells lacking the IME2 gene (ime2Δ), supporting an indirect role of Ime2 in Sic1 destruction. We further examined global RNA expression comparing wild type and ime2Δ cells. Analysis of these expression data has provided evidence that Ime2 is required early in meiosis for normal transcription of many genes that are also periodically expressed during late G1 of the cell cycle.

Conclusions/significance: Our results place Ime2 at a position in the early meiotic pathway that lies upstream of the position occupied by Cln1,-2/Cdk1 in the analogous cell cycle pathway. Thus, Ime2 may functionally resemble Cln3/Cdk1 in promoting S phase entry, or it could play a role even further upstream in the corresponding meiotic cascade.

Download Citation (.nbib)

Reference Type: Journal Article | Research Support, N.I.H., Extramural
Authors: Brush GS, Najor NA, Dombkowski AA, Cukovic D, Sawarynski KE
Primary Lit For
Additional Lit For
Review For

Gene Ontology Annotations

Evidence ID	Analyze ID	Gene/Complex	Systematic Name/Complex Accession	Qualifier	Gene Ontology Term ID	Gene Ontology Term	Aspect	Annotation Extension	Evidence	Method	Source	Assigned On	Reference

Download (.txt)

Analyze

Phenotype Annotations

Evidence ID	Analyze ID	Gene	Gene Systematic Name	Phenotype	Experiment Type	Experiment Type Category	Mutant Information	Strain Background	Chemical	Details	Reference

Download (.txt)

Analyze

Disease Annotations

Evidence ID	Analyze ID	Gene	Gene Systematic Name	Disease Ontology Term	Disease Ontology Term ID	Qualifier	Evidence	Method	Source	Assigned On		Reference

Download (.txt)

Analyze

Regulation Annotations

Evidence ID	Analyze ID	Regulator	Regulator Systematic Name	Target	Target Systematic Name	Direction	Regulation of	Happens During	Regulator Type	Direction	Regulation Of	Happens During	Method	Evidence	Strain Background	Reference

Download (.txt)

Analyze

Post-translational Modifications

				Site		Modification	Modifier	Source	Reference

Download (.txt)

Analyze

Interaction Annotations

Genetic Interactions

Evidence ID	Analyze ID		Interactor	Interactor Systematic Name	Interactor	Interactor Systematic Name	Allele	Assay	Annotation	Action	Phenotype	SGA score	P-value	Source	Reference	Note

Download (.txt)

Analyze

Physical Interactions

Evidence ID	Analyze ID		Interactor	Interactor Systematic Name	Interactor	Interactor Systematic Name	Assay	Annotation	Action	Modification	Source	Reference	Note

Download (.txt)

Analyze

Functional Complementation Annotations

Complement ID	Locus ID	Gene	Species	Gene ID	Strain background	Direction	Details	Source	Reference

Download (.txt)

Analyze

Published Datasets

Evidence ID	Analyze ID		Dataset	Description	Keywords	Number of Conditions	Reference

Download (.txt)

Analyze

Downloadable Files

Evidence ID	Analyze ID		File	Description

Download (.txt)

Analyze