Hannah R. Belsham
A Cdk1 phosphomimic mutant of MCAK impairs microtubule end recognition
Belsham, Hannah R.; Friel, Claire T.
Abstract
The microtubule depolymerising kinesin-13, MCAK, is phosphorylated at residue T537 by Cdk1. This is the only known phosphorylation site within MCAK’s motor domain. To understand the impact of phosphorylation by Cdk1 on microtubule depolymerisation activity, we have investigated the molecular mechanism of the phosphomimic mutant T537E. This mutant significantly impairs microtubule depolymerisation activity and when transfected into cells causes metaphase arrest and misaligned chromosomes. We show that the molecular mechanism underlying the reduced depolymerisation activity of this phosphomimic mutant is an inability to recognise the microtubule end. The microtubule-end residence time is reduced relative to wild-type MCAK, whereas the lattice residence time is unchanged by the phosphomimic mutation. Further, the microtubule-end specific stimulation of ADP dissociation, characteristic of MCAK, is abolished by this mutation. Our data shows that T537E is unable to distinguish between the microtubule end and the microtubule lattice.
Citation
Belsham, H. R., & Friel, C. T. (2017). A Cdk1 phosphomimic mutant of MCAK impairs microtubule end recognition. PeerJ, 5, Article e4034. https://doi.org/10.7717/peerj.4034
Journal Article Type | Article |
---|---|
Acceptance Date | Oct 24, 2017 |
Online Publication Date | Dec 6, 2017 |
Publication Date | Dec 6, 2017 |
Deposit Date | Nov 17, 2017 |
Publicly Available Date | Dec 6, 2017 |
Journal | PeerJ |
Electronic ISSN | 2167-8359 |
Publisher | PeerJ |
Peer Reviewed | Peer Reviewed |
Volume | 5 |
Article Number | e4034 |
DOI | https://doi.org/10.7717/peerj.4034 |
Keywords | MCAK; kinesin-13; Microtubule; Depolymerisation; Microtubule end recognition; Phosphomimic |
Public URL | https://nottingham-repository.worktribe.com/output/898653 |
Publisher URL | https://peerj.com/articles/4034/ |
Contract Date | Nov 17, 2017 |
Files
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Publisher Licence URL
https://creativecommons.org/licenses/by/4.0/
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