KIF14 and citron kinase act together to promote efficient cytokinesis

doi:10.1083/jcb.200511061

Published online 23 January 2006. doi:10.1083/jcb.200511061
The Rockefeller University Press, 0021-9525 $8.00
JCB, Volume 172, Number 3, 363-372

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Article

KIF14 and citron kinase act together to promote efficient cytokinesis

Ulrike Gruneberg¹, Rüdiger Neef², Xiuling Li¹, Eunice H.Y. Chan¹, Ravindra B. Chalamalasetty¹, Erich A. Nigg¹, and Francis A. Barr²

¹ Department of Cell Biology and ² Intracellular Protein Transport Group, Max-Planck-Institute of Biochemistry, 82152 Martinsried, Germany

Correspondence to Francis A. Barr: barr{at}biochem.mpg.de

Multiple mitotic kinesins and microtubule-associated proteins(MAPs) act in concert to direct cytokinesis (Glotzer, M. 2005.Science. 307:1735–1739). In anaphase cells, many of theseproteins associate with an antiparallel array of microtubulestermed the central spindle. The MAP and microtubule-bundlingprotein PRC1 (protein-regulating cytokinesis 1) is one of thekey molecules required for the integrity of this structure (Jiang,W., G. Jimenez, N.J. Wells, T.J. Hope, G.M. Wahl, T. Hunter,and R. Fukunaga. 1998. Mol. Cell. 2:877–885; Mollinari,C., J.P. Kleman, W. Jiang, G. Schoehn, T. Hunter, and R.L. Margolis.2002. J. Cell Biol. 157:1175–1186). In this study, weidentify an interaction between endogenous PRC1 and the previouslyuncharacterized kinesin KIF14 as well as other mitotic kinesins(MKlp1/CHO1, MKlp2, and KIF4) with known functions in cytokinesis(Hill, E., M. Clarke, and F.A. Barr. 2000. EMBO J. 19:5711–5719;Matuliene, J., and R. Kuriyama. 2002. Mol. Biol. Cell. 13:1832–1845;Kurasawa, Y., W.C. Earnshaw, Y. Mochizuki, N. Dohmae, and K.Todokoro. 2004. EMBO J. 23:3237–3248). We find that KIF14targets to the central spindle via its interaction with PRC1and has an essential function in cytokinesis. In KIF14-depletedcells, citron kinase but not other components of the centralspindle and cleavage furrow fail to localize. Furthermore, thelocalization of KIF14 and citron kinase to the central spindleand midbody is codependent, and they form a complex dependingon the activation state of citron kinase. Contrary to a previousstudy (Di Cunto, F., S. Imarisio, E. Hirsch, V. Broccoli, A.Bulfone, A. Migheli, C. Atzori, E. Turco, R. Triolo, G.P. Dotto,et al. 2000. Neuron. 28:115–127), we find a general requirementfor citron kinase in human cell division. Together, these findingsidentify a novel pathway required for efficient cytokinesis.

Abbreviations used in this paper: FHA, forkhead associated;INCENP, inner centromere protein; MAP, microtubule-associatedprotein; PRC1, protein-regulating cytokinesis 1; siRNA, smallinterfering RNA.

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