1. Academic Validation
  2. Aurora-B phosphorylation in vitro identifies a residue of survivin that is essential for its localization and binding to inner centromere protein (INCENP) in vivo

Aurora-B phosphorylation in vitro identifies a residue of survivin that is essential for its localization and binding to inner centromere protein (INCENP) in vivo

  • J Biol Chem. 2004 Feb 13;279(7):5655-60. doi: 10.1074/jbc.M311299200.
Sally P Wheatley 1 Alexander J Henzing Helen Dodson Walid Khaled William C Earnshaw
Affiliations

Affiliation

  • 1 Chromosome Structure Laboratory, Wellcome Centre for Cell Biology, Institute of Cell and Molecular Biology, University of Edinburgh, Mayfield Road, Edinburgh EH9 3JR, Scotland, United Kingdom. s.p.wheatley@sussex.ac.uk
Abstract

The chromosomal passengers, aurora-B kinase, inner centromere protein (INCENP), and Survivin, are essential proteins that have been implicated in the regulation of metaphase chromosome alignment, spindle checkpoint function, and cytokinesis. All three share a common pattern of localization, and it was recently demonstrated that aurora-B, INCENP, and Survivin are present in a complex in Xenopus eggs and Saccharomyces cerevisiae. The presence of aurora-B kinase in the complex and its ability to bind the Other components directly suggest that INCENP and Survivin could potentially be aurora-B substrates. This hypothesis was recently proven for INCENP in vitro. Here we report that human Survivin is specifically phosphorylated in vitro by aurora-B kinase at threonine 117 in its carboxyl alpha-helical coil. Mutation of threonine 117 to alanine prevents Survivin phosphorylation by aurora-B in vitro but does not alter its localization in HeLa cells. By contrast, a phospho-mimic, in which threonine 117 was mutated to glutamic acid, was unable to localize correctly at any stage in mitosis. Mutation at threonine 117 also prevented immunoprecipitation of INCENP with Survivin in vivo. These data suggest that phosphorylation of Survivin at threonine 117 by aurora-B may regulate targeting of Survivin, and possibly the entire passenger complex, in mammals.

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