| Literature DB >> 24949858 |
Kritica Arora1, Lama Talje2, Ana B Asenjo3, Parker Andersen2, Kaleem Atchia2, Monika Joshi1, Hernando Sosa3, John S Allingham4, Benjamin H Kwok5.
Abstract
The mitotic kinesin motor protein KIF14 is essential for cytokinesis during cell division and has been implicated in cerebral development and a variety of human cancers. Here we show that the mouse KIF14 motor domain binds tightly to microtubules and does not display typical nucleotide-dependent changes in this affinity. It also has robust ATPase activity but very slow motility. A crystal structure of the ADP-bound form of the KIF14 motor domain reveals a dramatically opened ATP-binding pocket, as if ready to exchange its bound ADP for Mg·ATP. In this state, the central β-sheet is twisted ~10° beyond the maximal amount observed in other kinesins. This configuration has only been seen in the nucleotide-free states of myosins-known as the "rigor-like" state. Fitting of this atomic model to electron density maps from cryo-electron microscopy indicates a distinct binding configuration of the motor domain to microtubules. We postulate that these properties of KIF14 are well suited for stabilizing midbody microtubules during cytokinesis.Entities:
Keywords: KIF14; crystal structure; kinesin; microtubules; motor protein
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Year: 2014 PMID: 24949858 DOI: 10.1016/j.jmb.2014.05.030
Source DB: PubMed Journal: J Mol Biol ISSN: 0022-2836 Impact factor: 5.469