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Functional characterization and comparative analysis of gene repression-mediating domains interacting with yeast pleiotropic corepressors Sin3, Cyc8 and Tup1

  • Transcriptional corepressors Sin3, Cyc8 and Tup1 are important for downregulation of gene expression by recruiting various histone deacetylases once they gain access to defined genomic locations by interaction with pathway-specific repressor proteins. In this work we systematically investigated whether 17 yeast repressor proteins (Cti6, Dal80, Fkh1, Gal80, Mig1, Mot3, Nrg1, Opi1, Rdr1, Rox1, Sko1, Ume6, Ure2, Xbp1, Yhp1, Yox1 and Whi5) representing several unrelated regulatory pathways are able to bind to Sin3, Cyc8 and Tup1. Our results show that paired amphipathic helices 1 and 2 (PAH1 and PAH2) of Sin3 are functionally redundant for some regulatory pathways. WD40 domains of Tup1 proved to be sufficient for interaction with repressor proteins. Using length variants of selected repressors, we mapped corepressor interaction domains (CIDs) in vitro and assayed gene repression in vivo. Systematic comparison of CID minimal sequences allowed us to define several related positional patterns of hydrophobic amino acids some of which could be confirmed as functionally supported by site-directed mutagenesis. Although structural predictions indicated that certain CIDs may be α-helical, most repression domains appear to be randomly structured and must be considered as intrinsically disordered regions (IDR) adopting a defined conformation only by interaction with a corepressor.

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Metadaten
Author: Julia Lettow, Felix Kliewe, Rasha Aref, Hans-Joachim Schüller
URN:urn:nbn:de:gbv:9-opus-108360
DOI:https://doi.org/10.1007/s00294-023-01262-6
ISSN:1432-0983
Parent Title (English):Current Genetics: Microorganisms and Organelles
Publisher:Springer Nature
Place of publication:Berlin
Document Type:Article
Language:English
Date of Publication (online):2023/03/01
Date of first Publication:2023/06/01
Release Date:2024/03/07
Tag:Corepressor; Cyc8; Gene repression; Interaction specificity; Saccharomyces cerevisiae; Sin3; Tup1
Volume:69
Issue:2-3
First Page:127
Last Page:139
Faculties:Mathematisch-Naturwissenschaftliche Fakultät / Interfakultäres Institut für Genetik und Funktionelle Genomforschung (MNF)
Collections:weitere DFG-förderfähige Artikel
Licence (German):License LogoCreative Commons - Namensnennung 4.0 International