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logo citeas Moschou, P. N., Gutierrez-Beltran, E., Bozhkov, P. V., & Smertenko, A. (2016, May). Separase Promotes Microtubule Polymerization by Activating CENP-E-Related Kinesin Kin7. Developmental Cell. Elsevier BV. http://doi.org/10.1016/j.devcel.2016.04.015
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Título

Separase promotes microtubulepolymerization by activating CENP-E-related kinesin Kin7

AutorMoschou, Panagiotis N.; Gutiérrez-Beltrán, Emilio CSIC ORCID ; Bozhkov, Peter V.; Smertenko, Andrei
FinanciadoresSwedish Research Council
Knut and Alice Wallenberg Foundation
Swedish Foundation for Strategic Research
National Institute of Food and Agriculture (US)
August Teodor Larsson Foundation
Olle Engkvist Foundation
The Erling-Persson Family Foundation
Fecha de publicación23-may-2016
EditorElsevier
CitaciónDevelopmental Cell 37(4): 350-361 (2016)
ResumenMicrotubules play an essential role in breaking cellular symmetry. We have previously shown that separase associates with microtubules and regulates microtubule-dependent establishment of cell polarity in Arabidopsis. However, separase lacks microtubule-binding activity, raising questions about mechanisms underlying this phenomenon. Here we report that the N-terminal non-catalytic domain of separase binds to the C-terminal tail domain of three homologs of the centromeric protein CENP-E Kinesin 7 (Kin7). Conformational changes of Kin7 induced upon binding to separase facilitate recruitment of Kin7/separase complex (KISC) onto microtubules. KISC operates independently of proteolytic activity of separase in promoting microtubule rescue and pauses, as well as in suppressing catastrophes. Genetic complementation experiments in conditional separase mutant rsw4 background demonstrate the importance of KISC for the establishment of cell polarity and for plant development. Our study establishes a mechanism governing microtubule dynamics via the separase-dependent activation of CENP-E-related kinesins.
Versión del editorhttps://doi.org/10.1016/j.devcel.2016.04.015
URIhttp://hdl.handle.net/10261/189966
DOI10.1016/j.devcel.2016.04.015
ISSN1534-5807
E-ISSN1878-1551
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