Phosphorylation of HsMis13 by Aurora B Kinase Is Essential for Assembly of Functional KinetochoreS
Chromosome movements in mitosis are orchestrated by dynamic interactions between spindle microtubules and the kinetochore, a multiprotein complex assembled onto centromeric DNA of the chromosome. Here we show that phosphorylation of human HsMis13 by Aurora B kinase is required for functional kinetoc...
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Veröffentlicht in: | The Journal of biological chemistry 2008-09, Vol.283 (39), p.26726-26736 |
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Sprache: | eng |
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Zusammenfassung: | Chromosome movements in mitosis are orchestrated by dynamic interactions
between spindle microtubules and the kinetochore, a multiprotein complex
assembled onto centromeric DNA of the chromosome. Here we show that
phosphorylation of human HsMis13 by Aurora B kinase is required for functional
kinetochore assembly in HeLa cells. Aurora B interacts with HsMis13
in
vitro
and
in vivo
. HsMis13 is a cognate substrate of Aurora B,
and the phosphorylation sites were mapped to Ser-100 and Ser-109. Suppression
of Aurora B kinase by either small interfering RNA or chemical inhibitors
abrogates the localization of HsMis13 but not HsMis12 to the kinetochore. In
addition, non-phosphorylatable but not wild type and phospho-mimicking HsMis13
failed to localize to the kinetochore, demonstrating the requirement of
phosphorylation by Aurora B for the assembly of HsMis13 to kinetochore. In
fact, localization of HsMis13 to the kinetochore is spatiotemporally regulated
by Aurora B kinase, which is essential for recruiting outer kinetochore
components such as Ndc80 components and CENP-E for functional kinetochore
assembly. Importantly, phospho-mimicking mutant HsMis13 restores the assembly
of CENP-E to the kinetochore, and tension developed across the sister
kinetochores in Aurora B-inhibited cells. Thus, we reason that HsMis13
phosphorylation by Aurora B is required for organizing a stable bi-oriented
microtubule kinetochore attachment that is essential for faithful chromosome
segregation in mitosis. |
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ISSN: | 0021-9258 1083-351X |
DOI: | 10.1074/jbc.M804207200 |