The Multi-subunit GID/CTLH E3 Ubiquitin Ligase Promotes Cell Proliferation and Targets the Transcription Factor Hbp1 for Degradation

Overview

Journal Elife

Specialty Biology

Date 2018 Jun 19

PMID 29911972

Citations 58

Authors

Fabienne Lampert

Diana Stafa

Algera Goga

Martin Varis Soste

Samuel Gilberto

Natacha Olieric

Paola Picotti

Markus Stoffel

Matthias Peter

Affiliations

Soon will be listed here.

Abstract

In yeast, the glucose-induced degradation-deficient (GID) E3 ligase selectively degrades superfluous gluconeogenic enzymes. Here, we identified all subunits of the mammalian GID/CTLH complex and provide a comprehensive map of its hierarchical organization and step-wise assembly. Biochemical reconstitution demonstrates that the mammalian complex possesses inherent E3 ubiquitin ligase activity, using Ube2H as its cognate E2. Deletions of multiple GID subunits compromise cell proliferation, and this defect is accompanied by deregulation of critical cell cycle markers such as the retinoblastoma (Rb) tumor suppressor, phospho-Histone H3 and Cyclin A. We identify the negative regulator of pro-proliferative genes Hbp1 as a GID/CTLH proteolytic substrate. Indeed, Hbp1 accumulates in cells lacking GID/CTLH activity, and Hbp1 physically interacts and is ubiquitinated in vitro by reconstituted GID/CTLH complexes. Our biochemical and cellular analysis thus demonstrates that the GID/CTLH complex prevents cell cycle exit in G1, at least in part by degrading Hbp1.

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