Literature DB >> 15247293

Mechanistic analysis of the mitotic kinesin Eg5.

Jared C Cochran1, Christopher A Sontag, Zoltan Maliga, Tarun M Kapoor, John J Correia, Susan P Gilbert.   

Abstract

Eg5 is a slow, plus-end-directed microtubule-based motor of the BimC kinesin family that is essential for bipolar spindle formation during eukaryotic cell division. We have analyzed two human Eg5/KSP motors, Eg5-367 and Eg5-437, and both are monomeric based on results from sedimentation velocity and sedimentation equilibrium centrifugation as well as analytical gel filtration. The steady-state parameters were: for Eg5-367: k(cat) = 5.5 s(-1), K(1/2,Mt) = 0.7 microm, and K(m,ATP) = 25 microm; and for Eg5-437: k(cat) = 2.9 s(-1), K(1/2,Mt) = 4.5 microm, and K(m,ATP) = 19 microm. 2'(3')-O-(N-Methylanthraniloyl)-ATP (mantATP) binding was rapid at 2-3 microm(-1)s(-1), followed immediately by ATP hydrolysis at 15 s(-1). ATP-dependent Mt.Eg5 dissociation was relatively slow and rate-limiting at 8 s(-1) with mantADP release at 40 s(-1). Surprisingly, Eg5-367 binds microtubules more effectively (11 microm(-1)s(-1)) than Eg5-437 (0.7 microm(-1)s(-1)), consistent with the steady-state K(1/2,Mt) and the mantADP release K(1/2,Mt). These results indicate that the ATPase pathway for monomeric Eg5 is more similar to conventional kinesin than the spindle motors Ncd and Kar3, where ADP product release is rate-limiting for steady-state turnover.

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Year:  2004        PMID: 15247293      PMCID: PMC1356567          DOI: 10.1074/jbc.M404203200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  86 in total

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  44 in total

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Journal:  J Biol Chem       Date:  2004-09-21       Impact factor: 5.157

2.  The loop 5 element structurally and kinetically coordinates dimers of the human kinesin-5, Eg5.

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9.  A novel small-molecule inhibitor reveals a possible role of kinesin-5 in anastral spindle-pole assembly.

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