Reference: Kuras L, et al. (2002) Dual regulation of the met4 transcription factor by ubiquitin-dependent degradation and inhibition of promoter recruitment. Mol Cell 10(1):69-80

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Abstract


The ubiquitin system has been recently implicated in various aspects of transcriptional regulation, including proteasome-dependent degradation of transcriptional activators. In yeast, the activator Met4 is inhibited by the SCF(Met30) ubiquitin ligase, which recognizes and oligo-ubiquitylates Met4. Here, we demonstrate that in minimal media, Met4 is ubiquitylated and rapidly degraded in response to methionine excess, whereas in rich media, Met4 is oligo-ubiquitylated but remains stable. In the latter growth condition, oligo-ubiquitylated Met4 is not recruited to MET gene promoters, but is recruited to the SAM genes, which are required for production of S-adenosylmethionine, an unstable metabolite that is not present in rich medium. Thus, ubiquitylation not only regulates Met4 by distinct degradation-dependent and -independent mechanisms, but also controls differential recruitment of a single transcription factor to distinct promoters, thereby diversifying transcriptional activator specificity.

Reference Type
Journal Article | Research Support, Non-U.S. Gov't
Authors
Kuras L, Rouillon A, Lee T, Barbey R, Tyers M, Thomas D
Primary Lit For
MET30 | SUA7 | MET4 | SCF-MET30 E3 ubiquitin ligase complex

Gene Ontology Annotations 2 entries for 1 gene


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Gene/ComplexQualifierGene Ontology TermAnnotation ExtensionEvidenceSourceAssigned On
SCF-MET30 E3 ubiquitin ligase complexinvolved inregulation of sulfur amino acid metabolic processBSRComplexPortal2014-10-16
SCF-MET30 E3 ubiquitin ligase complexinvolved inregulation of mitotic cell cycleBSRComplexPortal2014-10-16
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Interactor Interactor Allele Assay Annotation Action Phenotype SGA score P-value Source Reference

Physical Interactions 0 entries for 0 genes

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No physical interaction data for Kuras L, et al. (2002)
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