Aurora B kinase activation requires survivin priming phosphorylation by PLK1
Author(s) -
Youjun Chu,
Phil Y. Yao,
Wenwen Wang,
Dongmei Wang,
Zhikai Wang,
Liangyu Zhang,
Yuejia Huang,
Yuwen Ke,
Xia Ding,
Xuebiao Yao
Publication year - 2010
Publication title -
journal of molecular cell biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.825
H-Index - 62
eISSN - 1674-2788
pISSN - 1759-4685
DOI - 10.1093/jmcb/mjq037
Subject(s) - aurora b kinase , plk1 , microbiology and biotechnology , cytokinesis , aurora kinase , centromere , kinetochore , aurora inhibitor , biology , spindle checkpoint , mitosis , spindle apparatus , chromosome segregation , multipolar spindles , aurora a kinase , genetics , cell division , cell cycle , chromosome , cell , gene
During cell division, chromosome segregation is orchestrated by the interaction of spindle microtubules with the centromere. Accurate attachment of spindle microtubules to kinetochore requires the chromosomal passenger of Aurora B kinase complex with borealin, INCENP and survivin (SUR). The current working model argues that SUR is responsible for docking Aurora B to the centromere whereas its precise role in Aurora B activation has been unclear. Here, we show that Aurora B kinase activation requires SUR priming phosphorylation at Ser20 which is catalyzed by polo-like kinase 1 (PLK1). Inhibition of PLK1 kinase activity or expression of non-phosphorylatable SUR mutant prevents Aurora B activation and correct spindle microtubule attachment. The PLK1-mediated regulation of Aurora B kinase activity was examined in real-time mitosis using fluorescence resonance energy transfer-based reporter and quantitative analysis of native Aurora B substrate phosphorylation. We reason that the PLK1-mediated priming phosphorylation is critical for orchestrating Aurora B activity in centromere which is essential for accurate chromosome segregation and faithful completion of cytokinesis.
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