1. Protein phosphatase 4 is phosphorylated and inactivated by Cdk in response to spindle toxins and interacts with γ-tubulin
- Author
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Patricia T.W. Cohen, Kathryn Campbell, Martin Voss, David G. Campbell, C. James Hastie, Mark Peggie, Alan R. Prescott, Nastja Saranzewa, and Cristina Martin-Granados
- Subjects
Cdk1 ,Molecular Sequence Data ,Spindle Apparatus ,Models, Biological ,paclitaxel ,chemistry.chemical_compound ,Tubulin ,Cyclin-dependent kinase ,Report ,CDC2 Protein Kinase ,Protein Interaction Mapping ,Phosphoprotein Phosphatases ,protein phosphatase 4 ,Humans ,Amino Acid Sequence ,Phosphorylation ,Protein Kinase Inhibitors ,Molecular Biology ,Mitosis ,Cyclin-dependent kinase 1 ,biology ,Nocodazole ,Cell Cycle ,Cell Biology ,Cell cycle ,3. Good health ,Cell biology ,Spindle apparatus ,Enzyme Activation ,Protein Subunits ,centrosome ,HEK293 Cells ,Biochemistry ,chemistry ,Centrosome ,biology.protein ,γ-tubulin ,HeLa Cells ,Protein Binding ,Subcellular Fractions ,Developmental Biology - Abstract
Many pharmaceuticals used to treat cancer target the cell cycle or mitotic spindle dynamics, such as the anti-tumor drug, paclitaxel, which stabilizes microtubules. Here we show that, in cells arrested in mitosis with the spindle toxins, nocodazole, or paclitaxel, the endogenous protein phosphatase 4 (Ppp4) complex Ppp4c-R2-R3A is phosphorylated on its regulatory (R) subunits, and its activity is inhibited. The phosphorylations are blocked by roscovitine, indicating that they may be mediated by Cdk1-cyclin B. Endogenous Ppp4c is enriched at the centrosomes in the absence and presence of paclitaxel, nocodazole, or roscovitine, and the activity of endogenous Ppp4c-R2-R3A is inhibited from G 1/S to the G 2/M phase of the cell cycle. Endogenous γ-tubulin and its associated protein, γ-tubulin complex protein 2, both of which are essential for nucleation of microtubules at centrosomes, interact with the Ppp4 complex. Recombinant γ-tubulin can be phosphorylated by Cdk1-cyclin B or Brsk1 and dephosphorylated by Ppp4c-R2-R3A in vitro. The data indicate that Ppp4c-R2-R3A regulates microtubule organization at centrosomes during cell division in response to stress signals such as spindle toxins, paclitaxel, and nocodazole, and that inhibition of the Ppp4 complex may be advantageous for treatment of some cancers.
- Published
- 2013
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