| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2040573 | Cell Reports | 2015 | 8 Pages |
•Microtubule binding by the CC domain of INCENP promotes CPC midzone localization•The CPC multimerizes via the CEN box of INCENP•Multimerization of the CPC increases the microtubule binding affinity of INCENP•Centromere binding outcompetes microtubule binding of the CPC before anaphase
SummaryThe chromosomal passenger complex is essential for error-free chromosome segregation and proper execution of cytokinesis. To coordinate nuclear division with cytoplasmic division, its enzymatic subunit, Aurora B, relocalizes from centromeres in metaphase to the spindle midzone in anaphase. In budding yeast, this requires dephosphorylation of the microtubule-binding (MTB) domain of the INCENP analog Sli15. The mechanistic basis for this relocalization in metazoans is incompletely understood. We demonstrate that the putative coiled-coil domain within INCENP drives midzone localization of Aurora B via a direct, electrostatic interaction with microtubules. Furthermore, we provide evidence that the CPC multimerizes via INCENP’s centromere-targeting domain (CEN box), which increases the MTB affinity of INCENP. In (pro)metaphase, the MTB affinity of INCENP is outcompeted by the affinity of its CEN box for centromeres, while at anaphase onset—when the histone mark H2AT120 is dephosphorylated—INCENP and Aurora B switch from centromere to microtubule localization.
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