Centrobin regulates the assembly of functional mitotic spindles

被引:0
|
作者
J M Jeffery
A J Urquhart
V N Subramaniam
R G Parton
K K Khanna
机构
[1] Signal Transduction Laboratory,Cancer and Cell Biology Division
[2] Queensland Institute of Medical Research,Cancer and Cell Biology Division
[3] Membrane Transport Laboratory,Molecular Cell Biology Division
[4] Queensland Institute of Medical Research,undefined
[5] Institute for Molecular Bioscience,undefined
[6] The University of Queensland,undefined
[7] Centre for Microscopy and Microanalysis,undefined
[8] The University of Queensland,undefined
来源
Oncogene | 2010年 / 29卷
关键词
Centrobin; mitosis; mitotic spindle; spindle assembly checkpoint;
D O I
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中图分类号
学科分类号
摘要
The proper function of the spindle is crucial to the high fidelity of chromosome segregation and is indispensable for tumor suppression in humans. Centrobin is a recently identified centrosomal protein that has a role in stabilizing the microtubule structure. Here we functionally characterize the defects in centrosome integrity and spindle assembly in Centrobin-depleted cells. Centrobin-depleted cells show a range of spindle abnormalities including unfocused poles that are not associated with centrosomes, S-shaped spindles and mini spindles. These cells undergo mitotic arrest and subsequently often die by apoptosis, as determined by live cell imaging. Co-depletion of Mad2 relieves the mitotic arrest, indicating that cells arrest due to a failure to silence the spindle checkpoint in metaphase. Consistent with this, Centrobin-depleted metaphase cells stained positive for BubR1 and BubR1 S676. Staining with a panel of centrosome markers showed a loss of centrosome anchoring to the mitotic spindle. Furthermore, these cells show less cold-stable microtubules and a shorter distance between kinetochore pairs. These results show a requirement of Centrobin in maintaining centrosome integrity, which in turn promotes anchoring of mitotic spindle to the centrosomes. Furthermore, this anchoring is required for the stability of microtubule–kinetochore attachments and biogenesis of tension-ridden and properly functioning mitotic spindle.
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页码:2649 / 2658
页数:9
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