Mammalian Cdh1/Fzr mediates its own degradation.
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Journal: 2005/July - EMBO Journal
ISSN: 0261-4189
Abstract:
The Anaphase-Promoting Complex/Cyclosome (APC/C) ubiquitin ligase mediates degradation of cell cycle proteins during mitosis and G1. Cdc20/Fzy and Cdh1/Fzr are substrate-specific APC/C activators. The level of mammalian Cdh1 is high in mitosis, but it is inactive and does not bind the APC/C. We show that when Cdh1 is active in G1 and G0, its levels are considerably lower and almost all of it is APC/C associated. We demonstrate that Cdh1 is subject to APC/C-specific degradation in G1 and G0, and that this degradation depends upon two RXXL-type destruction boxes. We further demonstrate that addition of Cdh1 to Xenopus interphase extracts, which have an inactive APC/C, activates it to degrade Cdh1. These observations indicate that Cdh1 mediates its own degradation by activating the APC/C to degrade itself. Elevated levels of Cdh1 are deleterious for cell cycle progression in various organisms. This auto-regulation of Cdh1 could thus play a role in ensuring that the level of Cdh1 is reduced during G1 and G0, allowing it to be switched off at the correct time.
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EMBO J 23(7): 1619-1626
PMID: 15029244

Mammalian Cdh1/Fzr mediates its own degradation

Department of Genetics, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem, Israel
Unit of Biochemistry, The Rappaport Institute of Medical Research, The Technion-Israel Institute for Technology, Haifa, Israel
Cancer Research-UK, Clare Hall Laboratories, South Mimms, Herts, UK
Protein Purification Unit, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem, Israel
School of Engineering, Bar Ilan University, Ramat Gan, Israel
Department of Genetics, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Jerusalem 91904, Israel. Tel: +972 2 6585123; Fax: +972 2 6586975; E-mail: li.ca.ijuh.cc@siednarb
Received 2003 Jul 15; Accepted 2004 Feb 9.
Copyright © 2004, European Molecular Biology Organization

Abstract

The Anaphase-Promoting Complex/Cyclosome (APC/C) ubiquitin ligase mediates degradation of cell cycle proteins during mitosis and G1. Cdc20/Fzy and Cdh1/Fzr are substrate-specific APC/C activators. The level of mammalian Cdh1 is high in mitosis, but it is inactive and does not bind the APC/C. We show that when Cdh1 is active in G1 and G0, its levels are considerably lower and almost all of it is APC/C associated. We demonstrate that Cdh1 is subject to APC/C-specific degradation in G1 and G0, and that this degradation depends upon two RXXL-type destruction boxes. We further demonstrate that addition of Cdh1 to Xenopus interphase extracts, which have an inactive APC/C, activates it to degrade Cdh1. These observations indicate that Cdh1 mediates its own degradation by activating the APC/C to degrade itself. Elevated levels of Cdh1 are deleterious for cell cycle progression in various organisms. This auto-regulation of Cdh1 could thus play a role in ensuring that the level of Cdh1 is reduced during G1 and G0, allowing it to be switched off at the correct time.

Keywords: APC/C, cyclosome, destruction box, fizzy, fizzy- related
Abstract

Acknowledgments

We thank Avram Hershko and Tim Hunt for their generous help, Julian Gannon for Cdh1 antibodies, Miriam Broit for technical help and Christian Lehner and Jamie Simpson for fruitful discussions. This work was funded by the German Israeli Foundation (GIF 658/2000) and the Association for International Cancer Research (AICR). MB is the recipient of an ASCBI fellowship of the International Union Against Cancer (UICC).

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