Target genes of the protooncogene c-myc are implicated in cell cycle and growth control, yet the linkage of both is still unexplored. Here, we show that the products of the nucleolar target genes Pes1 and Bop1 form a stable complex with a novel member, WDR12 (PeBoW complex). Endogenous WDR12, a WD40 repeat protein, is crucial for processing of the 32S precursor ribosomal RNA (rRNA) and cell proliferation. Further, a conditionally expressed dominant-negative mutant of WDR12 also blocks rRNA processing and induces a reversible cell cycle arrest. Mutant WDR12 triggers accumulation of p53 in a p19ARF-independent manner in proliferating cells but not in quiescent cells. Interestingly, a potential homologous complex of Pes1–Bop1–WDR12 in yeast (Nop7p–Erb1p–Ytm1p) is involved in the control of ribosome biogenesis and S phase entry. In conclusion, the integrity of the PeBoW complex is required for ribosome biogenesis and cell proliferation in mammalian cells.
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1 August 2005
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July 25 2005
Mammalian WDR12 is a novel member of the Pes1–Bop1 complex and is required for ribosome biogenesis and cell proliferation
Michael Hölzel,
Michael Hölzel
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
4Department of Internal Medicine III, University Hospital Grosshadern, Ludwig-Maximilians-University, 81377 Munich, Germany
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Michaela Rohrmoser,
Michaela Rohrmoser
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Martin Schlee,
Martin Schlee
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Thomas Grimm,
Thomas Grimm
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Thomas Harasim,
Thomas Harasim
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Anastassia Malamoussi,
Anastassia Malamoussi
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Anita Gruber-Eber,
Anita Gruber-Eber
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Elisabeth Kremmer,
Elisabeth Kremmer
2Institute of Molecular Immunology, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Wolfgang Hiddemann,
Wolfgang Hiddemann
3Clinical Cooperative Group Acute Leukemia, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
4Department of Internal Medicine III, University Hospital Grosshadern, Ludwig-Maximilians-University, 81377 Munich, Germany
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Georg W. Bornkamm,
Georg W. Bornkamm
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Dirk Eick
Dirk Eick
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
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Michael Hölzel
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
4Department of Internal Medicine III, University Hospital Grosshadern, Ludwig-Maximilians-University, 81377 Munich, Germany
Michaela Rohrmoser
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Martin Schlee
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Thomas Grimm
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Thomas Harasim
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Anastassia Malamoussi
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Anita Gruber-Eber
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Elisabeth Kremmer
2Institute of Molecular Immunology, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Wolfgang Hiddemann
3Clinical Cooperative Group Acute Leukemia, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
4Department of Internal Medicine III, University Hospital Grosshadern, Ludwig-Maximilians-University, 81377 Munich, Germany
Georg W. Bornkamm
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Dirk Eick
1Institute of Clinical Molecular Biology and Tumour Genetics, National Research Center for Environment and Health (GSF), 81377 Munich, Germany
Correspondence to Dirk Eick: [email protected]
Abbreviations used in this paper: rRNA, ribosomal RNA; siRNA, small interfering RNA.
Received:
January 27 2005
Accepted:
June 21 2005
Online ISSN: 1540-8140
Print ISSN: 0021-9525
The Rockefeller University Press
2005
J Cell Biol (2005) 170 (3): 367–378.
Article history
Received:
January 27 2005
Accepted:
June 21 2005
Citation
Michael Hölzel, Michaela Rohrmoser, Martin Schlee, Thomas Grimm, Thomas Harasim, Anastassia Malamoussi, Anita Gruber-Eber, Elisabeth Kremmer, Wolfgang Hiddemann, Georg W. Bornkamm, Dirk Eick; Mammalian WDR12 is a novel member of the Pes1–Bop1 complex and is required for ribosome biogenesis and cell proliferation . J Cell Biol 1 August 2005; 170 (3): 367–378. doi: https://doi.org/10.1083/jcb.200501141
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