Literature DB >> 17509883

Nonredundant functions of Kinesin-13s during meiotic spindle assembly.

Ryoma Ohi1, Kendra Burbank, Qing Liu, Timothy J Mitchison.   

Abstract

Spatiotemporal control of microtubule depolymerization during cell division underlies the construction and dynamics of mitotic and meiotic spindles. Owing to their potent ability to disassemble microtubules, Kinesin-13s constitute an important class of microtubule destabilizing factors. Unfertilized Xenopus eggs, similar to other metazoan cells, contain the prototypical Kinesin-13 MCAK as well as a second family member, XKIF2. Here, we compare the roles of MCAK and XKIF2 during spindle assembly in Xenopus extracts. We find that although MCAK and XKIF2 have similar localization and biochemical properties, XKIF2 is not required for spindle assembly and, further, cannot substitute for MCAK. Altering dosage of the two kinesins demonstrates that spindle length is exquisitely sensitive to MCAK concentration but not XKIF2 concentration. Finally, we demonstrate that the rate of poleward microtubule flux in Xenopus-extract spindles is unaffected by XKIF2 depletion and is only modestly sensitive to reduction of MCAK action. We suggest that, in contrast to models proposed for mammalian somatic cell and embryonic Drosophila spindles, Kinesin-13s do not play a central role in poleward flux by depolymerizing minus ends. Rather, MCAK, but not XKIF2, plays a central role in regulating dynamic instability of plus ends and controls spindle length by that mechanism.

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Year:  2007        PMID: 17509883     DOI: 10.1016/j.cub.2007.04.057

Source DB:  PubMed          Journal:  Curr Biol        ISSN: 0960-9822            Impact factor:   10.834


  53 in total

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5.  Op18 reveals the contribution of nonkinetochore microtubules to the dynamic organization of the vertebrate meiotic spindle.

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6.  Using micromanipulation to analyze control of vertebrate meiotic spindle size.

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7.  Meiosis I in Xenopus oocytes is not error-prone despite lacking spindle assembly checkpoint.

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8.  Signaling-dependent phosphorylation of mitotic centromere-associated kinesin regulates microtubule depolymerization and its centrosomal localization.

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9.  Motor-dependent microtubule disassembly driven by tubulin tyrosination.

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10.  Fast microtubule dynamics in meiotic spindles measured by single molecule imaging: evidence that the spindle environment does not stabilize microtubules.

Authors:  Daniel J Needleman; Aaron Groen; Ryoma Ohi; Tom Maresca; Leonid Mirny; Tim Mitchison
Journal:  Mol Biol Cell       Date:  2009-11-25       Impact factor: 4.138

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