Author
Listed:
- Yogesh Kulathu
(MRC Laboratory of Molecular Biology
Present address: MRC Protein Phosphorylation Unit, College of Life Sciences, University of Dundee, Dow Street, Dundee DD1 5EH, UK)
- Francisco J. Garcia
(The Scripps Research Institute)
- Tycho E. T. Mevissen
(MRC Laboratory of Molecular Biology)
- Martin Busch
(MRC Laboratory of Molecular Biology
Present address: Rudolf-Virchow-Centre, University of Würzburg, Josef-Schneider-Straße 2, 97080 Würzburg, Germany)
- Nadia Arnaudo
(MRC Laboratory of Molecular Biology)
- Kate S. Carroll
(The Scripps Research Institute)
- David Barford
(Institute of Cancer Research)
- David Komander
(MRC Laboratory of Molecular Biology)
Abstract
Protein ubiquitination is a highly versatile post-translational modification that regulates as diverse processes as protein degradation and kinase activation. Deubiquitinases hydrolyse ubiquitin modifications from proteins and are hence key regulators of the ubiquitin system. Ovarian tumour deubiquitinases comprise a family of fourteen human enzymes, many of which regulate cellular signalling pathways. Ovarian tumour deubiquitinases are cysteine proteases that cleave polyubiquitin chains in vitro and in cells, but little is currently known about their regulation. Here we show that ovarian tumour deubiquitinases are susceptible to reversible oxidation of the catalytic cysteine residue. High-resolution crystal structures of the catalytic domain of A20 in four different oxidation states reveal that the reversible form of A20 oxidation is a cysteine sulphenic acid intermediate, which is stabilised by the architecture of the catalytic centre. Using chemical tools to detect sulphenic acid intermediates, we show that many ovarian tumour deubiquitinases undergo reversible oxidation upon treatment with H2O2, revealing a new mechanism to regulate deubiquitinase activity.
Suggested Citation
Yogesh Kulathu & Francisco J. Garcia & Tycho E. T. Mevissen & Martin Busch & Nadia Arnaudo & Kate S. Carroll & David Barford & David Komander, 2013.
"Regulation of A20 and other OTU deubiquitinases by reversible oxidation,"
Nature Communications, Nature, vol. 4(1), pages 1-9, June.
Handle:
RePEc:nat:natcom:v:4:y:2013:i:1:d:10.1038_ncomms2567
DOI: 10.1038/ncomms2567
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