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Article
Nature 432, 980-987 (23 December 2004) | doi:10.1038/nature03160; Received 2 July 2004; Accepted 28 October 2004
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Assistant Professor
- University of Michigan
- Michigan, MI 48109 United States
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Genome-wide survey of protein kinases required for cell cycle progression
M. Bettencourt-Dias1, R. Giet1,2, R. Sinka1, A. Mazumdar1, W. G. Lock1, F. Balloux1, P. J. Zafiropoulos1, S. Yamaguchi3, S. Winter3, R. W. Carthew3, M. Cooper4, D. Jones4, L. Frenz4 & D. M. Glover1,4
- Cancer Research UK Cell Cycle Genetics Research Group, University of Cambridge, Department of Genetics, Downing Street, Cambridge CB2 3EH, UK
- CNRS UMR 6061 Université de Rennes 1, Equipe Labellisée Ligue Nationale Contre le Cancer, Groupe Cycle Cellulaire, IFR97, 2 avenue du Pr Léon Bernard, 35043 Rennes, France
- Department of Biochemistry, Molecular Biology and Cell Biology, Northwestern University, Chicago, Illinois 60208, USA
- Polgen Division, Cyclacel Ltd, Babraham Science Park, Babraham, Cambridge CB4 2AT, UK
Correspondence to: M. Bettencourt-Dias1D. M. Glover1,4 Email: mbcd2@cam.ac.uk
Email: dmg25@mole.bio.cam.ac.uk
Abstract
Cycles of protein phosphorylation are fundamental in regulating the progression of the eukaryotic cell through its division cycle. Here we test the complement of Drosophila protein kinases (kinome) for cell cycle functions after gene silencing by RNA-mediated interference. We observed cell cycle dysfunction upon downregulation of 80 out of 228 protein kinases, including most kinases that are known to regulate the division cycle. We find new enzymes with cell cycle functions; some of these have family members already known to phosphorylate microtubules, actin or their associated proteins. Additionally, depletion of several signalling kinases leads to specific mitotic aberrations, suggesting novel roles for familiar enzymes. The survey reveals the inter-digitation of systems that monitor cellular physiology, cell size, cellular stress and signalling processes with the basic cell cycle regulatory machinery.
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