Sequestration of Polo kinase to microtubules by phosphopriming-independent binding to Map205 is relieved by phosphorylation at a CDK site in mitosis
Abstract
The conserved Polo kinase controls multiple events in mitosis and cytokinesis. Although Polo-like kinases are regulated by phosphorylation and proteolysis, control of subcellular localization plays a major role in coordinating their mitotic functions. This is achieved largely by the Polo-Box Domain, which binds prephosphorylated targets. However, it remains unclear whether and how Polo might interact with partner proteins when priming mitotic kinases are inactive. Here we show that Polo associates with microtubules in interphase and cytokinesis, through a strong interaction with the microtubule-associated protein Map205. Surprisingly, this interaction does not require priming phosphorylation of Map205, and the Polo-Box Domain of Polo is required but not sufficient for this interaction. Moreover, phosphorylation of Map205 at a CDK site relieves this interaction. Map205 can stabilize Polo and inhibit its cellular activity in vivo. In syncytial embryos, the centrosome defects observed in polo hypomorphs are enhanced by overexpression of Map205 and suppressed by its deletion. We propose that Map205-dependent targeting of Polo to microtubules provides a stable reservoir of Polo that can be rapidly mobilized by the activity of Cdk1 at mitotic entry.
Additional Information
© 2008, Cold Spring Harbor Laboratory Press. The Authors acknowledge that six months after the full-issue publication date, the Article will be distributed under a Creative Commons CC-BY-NC License (Attribution-NonCommercial 4.0 International License, http://creativecommons.org/licenses/by-nc/4.0/). Received May 9, 2008; revised version accepted August 7, 2008. We thank Michaela Scigelova and Gary Woffendin from ThermoFisher for performing the ETD mass spectrometry experiments for phosphorylation site mapping and Svenja Hester for protein identification. We thank Andrea Pereira for his generous gift of anti-Map205 antibodies, Hiro Ohkura for the map205-null fly line, Matthew Savoian for precious help with the microcopy, and members of the Glover laboratory for useful advice and discussions. V.A. was supported by long-term fellowships from the European Molecular Biology Organization and from the Human Science Frontier Program. This work was also supported by CR-UK, BBSRC, and MRC grant G0501718.Attached Files
Published - Genes_Dev.-2008-Archambault-2707-20.pdf
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Supplemental Material - ArchambaultSuppFigS12.doc
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Additional details
- PMCID
- PMC2559908
- Eprint ID
- 104859
- Resolver ID
- CaltechAUTHORS:20200807-170353006
- European Molecular Biology Organization (EMBO)
- Human Frontier Science Program
- Cancer Research UK
- Biotechnology and Biological Sciences Research Council (BBSRC)
- Medical Research Council (UK)
- G0501718
- Created
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2020-08-19Created from EPrint's datestamp field
- Updated
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2021-11-16Created from EPrint's last_modified field