Normal cell cycle progression requires negative regulation of E2F1 by Groucho during S phase and its relief at G2 phase

Author:

Bar-Cohen Shaked1,Martínez Quiles María Lorena2,Baskin Alexey3,Dawud Ruba1,Jennings Barbara H.2ORCID,Paroush Ze'ev1ORCID

Affiliation:

1. Institute for Medical Research Israel-Canada, Faculty of Medicine, The Hebrew University 1 Department of Developmental Biology and Cancer Research , , Jerusalem 91120 , Israel

2. Oxford Brookes University 2 Department of Biological and Medical Sciences , , Oxford OX3 0BP , UK

3. The Institute of Life Science, The Hebrew University of Jerusalem 3 Department of Biological Chemistry , , Jerusalem 91904 , Israel

Abstract

ABSTRACT The cell cycle depends on a sequence of steps that are triggered and terminated via the synthesis and degradation of phase-specific transcripts and proteins. Although much is known about how stage-specific transcription is activated, less is understood about how inappropriate gene expression is suppressed. Here, we demonstrate that Groucho, the Drosophila orthologue of TLE1 and other related human transcriptional corepressors, regulates normal cell cycle progression in vivo. We show that, although Groucho is expressed throughout the cell cycle, its activity is selectively inactivated by phosphorylation, except in S phase when it negatively regulates E2F1. Constitutive Groucho activity, as well as its depletion and the consequent derepression of e2f1, cause cell cycle phenotypes. Our results suggest that Cdk1 contributes to phase-specific phosphorylation of Groucho in vivo. We propose that Groucho and its orthologues play a role in the metazoan cell cycle that may explain the links between TLE corepressors and several types of human cancer.

Funder

Israel Science Foundation

Hebrew University of Jerusalem Faculty of Medicine

The Jan M. and Eugenia Krol Charitable Foundation

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

Reference81 articles.

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