2004
DOI: 10.1016/s1534-5807(04)00025-5
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Aurora B Regulates MCAK at the Mitotic Centromere

Abstract: Chromosome orientation and alignment within the mitotic spindle requires the Aurora B protein kinase and the mitotic centromere-associated kinesin (MCAK). Here, we report the regulation of MCAK by Aurora B. Aurora B inhibited MCAK's microtubule depolymerizing activity in vitro, and phospho-mimic (S/E) mutants of MCAK inhibited depolymerization in vivo. Expression of either MCAK (S/E) or MCAK (S/A) mutants increased the frequency of syntelic microtubule-kinetochore attachments and mono-oriented chromosomes. MCA… Show more

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Cited by 500 publications
(618 citation statements)
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“…This is consistent with the complex localization of MCAK in the spindle and the highly complicated phosphorregulatory schemes that regulate its localization and activity at centromeres and at spindle poles (Andrews et al, 2004;Gorbsky, 2004;Lan et al, 2004;Ohi et al, 2004;Knowlton et al, 2006;Zhang et al, 2007Zhang et al, , 2008. This suggests that MCAK is responsible for preferentially altering the dynamics individual MT subclasses and raises the important question of how other MT dynamics effectors contribute to the control of spindle MT subclasses.…”
Section: Control Of Kinetochore Mt Dynamicssupporting
confidence: 76%
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“…This is consistent with the complex localization of MCAK in the spindle and the highly complicated phosphorregulatory schemes that regulate its localization and activity at centromeres and at spindle poles (Andrews et al, 2004;Gorbsky, 2004;Lan et al, 2004;Ohi et al, 2004;Knowlton et al, 2006;Zhang et al, 2007Zhang et al, , 2008. This suggests that MCAK is responsible for preferentially altering the dynamics individual MT subclasses and raises the important question of how other MT dynamics effectors contribute to the control of spindle MT subclasses.…”
Section: Control Of Kinetochore Mt Dynamicssupporting
confidence: 76%
“…Our data are consistent with the recent findings of Wordeman et al (2007), who propose an attractive idea that the role of MCAK is to loosen up MT ends to facilitate directional coordination of chromosome motility and MT release. Another interesting observation is that although it has been clearly established that MCAK is a substrate of Aurora B kinase (Andrews et al, 2004;Lan et al, 2004;Sampath et al, 2004;Zhang et al, 2007), the magnitude of the effects of MCAK inhibition versus Aurora B inhibition on the t 1/2 value of the K-fiber strongly supports the idea that Aurora B causes release of aberrant MT attachments primarily through a mechanism that does not rely solely on MCAK DeLuca et al, 2006;Wordeman et al, 2007).…”
Section: Control Of Kinetochore Mt Dynamicsmentioning
confidence: 93%
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“…Consequently, knockdown or inhibition of Aurora B or any of the other subunits of the CPC results in chromosome congression defects, kinetochore-microtubule attachment errors, lagging chromosomes in anaphase, and failure of cytokinesis (Vagnarelli and Earnshaw, 2004;Tanaka, 2005). Consistent with the idea that the localization of the CPC is important for target recognition by its kinase subunit, Aurora B has been demonstrated to phosphorylate proteins at the centromere, such as CENP-A and mitotic centromere-associated kinesin (MCAK) (Zeitlin et al, 2001;Andrews et al, 2004;Lan et al, 2004;Ohi et al, 2004), and at the central spindle and midbody, e.g., Mklp1, MgcRacGap, and vimentin (Goto et al, 2003;Minoshima et al, 2003;Guse et al, 2005). Yet, the molecular details of how phosphorylation by Aurora B influences its different substrates and thus regulates the different stages of the cell cycle are still not clear.…”
Section: Introductionmentioning
confidence: 86%
“…For example, the localization of metazoan MKLP1, a kinesin essential for central spindle formation, is dependent on IN-CENP function (Zhu et al, 2005). Similarly, the activity of vertebrate MCAK, a microtubule-depolymerizing protein, is regulated through its phosphorylation by Aurora B kinase (Andrews et al, 2004;Lan et al, 2004). Although a Dictyostelium homolog of MCAK has yet to be identified, the homolog of MCAK's antagonist, XMAP215/TOGp, has been characterized as the Dictyostelium DdCP224 protein.…”
Section: Ddincenp and Spindle Assemblymentioning
confidence: 99%