We have combined the proteomic analysis of Xenopus laevis in vitro–assembled chromosomes with RNA interference and live cell imaging in HeLa cells to identify novel factors required for proper chromosome segregation. The first of these is Bod1, a protein conserved throughout metazoans that associates with a large macromolecular complex and localizes with kinetochores and spindle poles during mitosis. Small interfering RNA depletion of Bod1 in HeLa cells produces elongated mitotic spindles with severe biorientation defects. Bod1-depleted cells form syntelic attachments that can oscillate and generate enough force to separate sister kinetochores, suggesting that microtubule–kinetochore interactions were intact. Releasing Bod1-depleted cells from a monastrol block increases the frequency of syntelic attachments and the number of cells displaying biorientation defects. Bod1 depletion does not affect the activity or localization of Aurora B but does cause mislocalization of the microtubule depolymerase mitotic centromere- associated kinesin and prevents its efficient phosphorylation by Aurora B. Therefore, Bod1 is a novel kinetochore protein that is required for the detection or resolution of syntelic attachments in mitotic spindles.
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22 October 2007
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October 15 2007
Bod1, a novel kinetochore protein required for chromosome biorientation
Iain M. Porter,
Iain M. Porter
1Division of Gene Regulation and Expression
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Sarah E. McClelland,
Sarah E. McClelland
3Chromosome Segregation Laboratory, Marie Curie Research Institute, Oxted, Surrey RH8 0TL, England, UK
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Guennadi A. Khoudoli,
Guennadi A. Khoudoli
1Division of Gene Regulation and Expression
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Christopher J. Hunter,
Christopher J. Hunter
2Medical Research Council Protein Phosphorylation Unit, College of Life Sciences, University of Dundee, Dundee DD1 5EH, Scotland, UK
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Jens S. Andersen,
Jens S. Andersen
4Center for Experimental Bioinformatics, University of Southern Denmark, DS-5230 Odense, Denmark
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Andrew D. McAinsh,
Andrew D. McAinsh
3Chromosome Segregation Laboratory, Marie Curie Research Institute, Oxted, Surrey RH8 0TL, England, UK
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J. Julian Blow,
J. Julian Blow
1Division of Gene Regulation and Expression
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Jason R. Swedlow
Jason R. Swedlow
1Division of Gene Regulation and Expression
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Iain M. Porter
1Division of Gene Regulation and Expression
Sarah E. McClelland
3Chromosome Segregation Laboratory, Marie Curie Research Institute, Oxted, Surrey RH8 0TL, England, UK
Guennadi A. Khoudoli
1Division of Gene Regulation and Expression
Christopher J. Hunter
2Medical Research Council Protein Phosphorylation Unit, College of Life Sciences, University of Dundee, Dundee DD1 5EH, Scotland, UK
Jens S. Andersen
4Center for Experimental Bioinformatics, University of Southern Denmark, DS-5230 Odense, Denmark
Andrew D. McAinsh
3Chromosome Segregation Laboratory, Marie Curie Research Institute, Oxted, Surrey RH8 0TL, England, UK
J. Julian Blow
1Division of Gene Regulation and Expression
Jason R. Swedlow
1Division of Gene Regulation and Expression
Correspondence to Jason R. Swedlow: [email protected]
Abbreviations used in this paper: ACA, anticentromere antibody; CENP, centromere protein; MCAK, mitotic centromere-associated kinesin; shRNA, short hairpin RNA.
Received:
April 17 2007
Accepted:
September 22 2007
Online ISSN: 1540-8140
Print ISSN: 0021-9525
The Rockefeller University Press
2007
J Cell Biol (2007) 179 (2): 187–197.
Article history
Received:
April 17 2007
Accepted:
September 22 2007
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Citation
Iain M. Porter, Sarah E. McClelland, Guennadi A. Khoudoli, Christopher J. Hunter, Jens S. Andersen, Andrew D. McAinsh, J. Julian Blow, Jason R. Swedlow; Bod1, a novel kinetochore protein required for chromosome biorientation . J Cell Biol 22 October 2007; 179 (2): 187–197. doi: https://doi.org/10.1083/jcb.200704098
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