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Curr Biol
2011 Jan 25;212:154-60. doi: 10.1016/j.cub.2010.12.038.
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A nonmotor microtubule binding site in kinesin-5 is required for filament crosslinking and sliding.
Weinger JS
,
Qiu M
,
Yang G
,
Kapoor TM
.
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Kinesin-5, a widely conserved motor protein required for assembly of the bipolar mitotic spindle in eukaryotes, forms homotetramers with two pairs of motor domains positioned at opposite ends of a dumbbell-shaped molecule [1-3]. It has long been assumed that this configuration of motor domains is the basis of kinesin-5's ability to drive relative sliding of microtubules [2, 4, 5]. Recently, it was suggested that in addition to the N-terminal motor domain, kinesin-5 also has a nonmotor microtubule binding site in its C terminus [6]. However, it is not known how the nonmotor domain contributes to motor activity, or how a kinesin-5 tetramer utilizes a combination of four motor and four nonmotor microtubule binding sites for its microtubule organizing functions. Here we show, in single molecule assays, that kinesin-5 homotetramers require the nonmotor C terminus for crosslinking and relative sliding of two microtubules. Remarkably, this domain enhances kinesin-5's microtubule binding without substantially reducing motor activity. Our results suggest that tetramerization of kinesin-5's low-processivity motor domains is not sufficient for microtubule sliding because the motor domains alone are unlikely to maintain persistent microtubule crosslinks. Rather, kinesin-5 utilizes nonmotor microtubule binding sites to tune its microtubule attachment dynamics, enabling it to efficiently align and sort microtubules during metaphase spindle assembly and function.
Braun,
The kinesin-14 Klp2 organizes microtubules into parallel bundles by an ATP-dependent sorting mechanism.
2009, Pubmed
Braun,
The kinesin-14 Klp2 organizes microtubules into parallel bundles by an ATP-dependent sorting mechanism.
2009,
Pubmed
Cole,
A "slow" homotetrameric kinesin-related motor protein purified from Drosophila embryos.
1994,
Pubmed
,
Xenbase
Cooper,
The diffusive interaction of microtubule binding proteins.
2009,
Pubmed
Crevel,
Kinetic evidence for low chemical processivity in ncd and Eg5.
1997,
Pubmed
,
Xenbase
Crevel,
Monastrol stabilises an attached low-friction mode of Eg5.
2004,
Pubmed
,
Xenbase
DeBonis,
Interaction of the mitotic inhibitor monastrol with human kinesin Eg5.
2003,
Pubmed
Fink,
The mitotic kinesin-14 Ncd drives directional microtubule-microtubule sliding.
2009,
Pubmed
Foster,
Kinetic studies of dimeric Ncd: evidence that Ncd is not processive.
2000,
Pubmed
Helenius,
The depolymerizing kinesin MCAK uses lattice diffusion to rapidly target microtubule ends.
2006,
Pubmed
Hentrich,
Microtubule organization by the antagonistic mitotic motors kinesin-5 and kinesin-14.
2010,
Pubmed
,
Xenbase
Hunter,
The kinesin-related protein MCAK is a microtubule depolymerase that forms an ATP-hydrolyzing complex at microtubule ends.
2003,
Pubmed
Jolly,
Kinesin-1 heavy chain mediates microtubule sliding to drive changes in cell shape.
2010,
Pubmed
,
Xenbase
Kapitein,
Microtubule cross-linking triggers the directional motility of kinesin-5.
2008,
Pubmed
,
Xenbase
Kapitein,
The bipolar mitotic kinesin Eg5 moves on both microtubules that it crosslinks.
2005,
Pubmed
,
Xenbase
Kapoor,
Eg5 is static in bipolar spindles relative to tubulin: evidence for a static spindle matrix.
2001,
Pubmed
,
Xenbase
Kapoor,
Probing spindle assembly mechanisms with monastrol, a small molecule inhibitor of the mitotic kinesin, Eg5.
2000,
Pubmed
,
Xenbase
Kashina,
A bipolar kinesin.
1996,
Pubmed
Kwok,
Allosteric inhibition of kinesin-5 modulates its processive directional motility.
2006,
Pubmed
,
Xenbase
Kwok,
The rate of bipolar spindle assembly depends on the microtubule-gliding velocity of the mitotic kinesin Eg5.
2004,
Pubmed
,
Xenbase
Luo,
ATP-competitive inhibitors of the mitotic kinesin KSP that function via an allosteric mechanism.
2007,
Pubmed
Maliga,
Evidence that monastrol is an allosteric inhibitor of the mitotic kinesin Eg5.
2002,
Pubmed
,
Xenbase
Ponti,
Computational analysis of F-actin turnover in cortical actin meshworks using fluorescent speckle microscopy.
2003,
Pubmed
Sawin,
Mitotic spindle organization by a plus-end-directed microtubule motor.
1992,
Pubmed
,
Xenbase
Sharp,
The bipolar kinesin, KLP61F, cross-links microtubules within interpolar microtubule bundles of Drosophila embryonic mitotic spindles.
1999,
Pubmed
Tao,
A homotetrameric kinesin-5, KLP61F, bundles microtubules and antagonizes Ncd in motility assays.
2006,
Pubmed
Valentine,
Individual dimers of the mitotic kinesin motor Eg5 step processively and support substantial loads in vitro.
2006,
Pubmed
van den Wildenberg,
The homotetrameric kinesin-5 KLP61F preferentially crosslinks microtubules into antiparallel orientations.
2008,
Pubmed
