Müller H, et al. (2022)

Reference: Müller H, et al. (2022) Proteomic consequences of TDA1 deficiency in Saccharomyces cerevisiae: Protein kinase Tda1 is essential for Hxk1 and Hxk2 serine 15 phosphorylation. Sci Rep 12(1):18084

Reference Help

Abstract

Hexokinase 2 (Hxk2) of Saccharomyces cerevisiae is a dual function hexokinase, acting as a glycolytic enzyme and being involved in the transcriptional regulation of glucose-repressible genes. Relief from glucose repression is accompanied by phosphorylation of Hxk2 at serine 15, which has been attributed to the protein kinase Tda1. To explore the role of Tda1 beyond Hxk2 phosphorylation, the proteomic consequences of TDA1 deficiency were investigated by difference gel electrophoresis (2D-DIGE) comparing a wild type and a Δtda1 deletion mutant. To additionally address possible consequences of glucose repression/derepression, both were grown at 2% and 0.1% (w/v) glucose. A total of eight protein spots exhibiting a minimum twofold enhanced or reduced fluorescence upon TDA1 deficiency was detected and identified by mass spectrometry. Among the spot identities are-besides the expected Hxk2-two proteoforms of hexokinase 1 (Hxk1). Targeted proteomics analyses in conjunction with 2D-DIGE demonstrated that TDA1 is indispensable for Hxk2 and Hxk1 phosphorylation at serine 15. Thirty-six glucose-concentration-dependent protein spots were identified. A simple method to improve spot quantification, approximating spots as rotationally symmetric solids, is presented along with new data on the quantities of Hxk1 and Hxk2 and their serine 15 phosphorylated forms at high and low glucose growth conditions. The Δtda1 deletion mutant exhibited no altered growth under high or low glucose conditions or on alternative carbon sources. Also, invertase activity, serving as a reporter for glucose derepression, was not significantly altered. Instead, an involvement of Tda1 in oxidative stress response is suggested.

Download Citation (.nbib)

Reference Type: Journal Article | Research Support, Non-U.S. Gov't
Authors: Müller H, Lesur A, Dittmar G, Gentzel M, Kettner K
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