A Spindle Checkpoint Arrest and a Cytokinesis Failure by the Dominant-negative Polo-box Domain of Plk1 in U-2 OS Cells

Polo kinases play critical roles for proper M-phase progression. They are characterized by the presence of two regions of homology in the C-terminal non-catalytic domain, termed polo-box 1 (PB1) and polo-box 2 (PB2). Here we demonstrate that both PB1 and PB2 are required for targeting the catalytic...

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Published in:The Journal of biological chemistry 2002-08, Vol.277 (35), p.32282-32293
Main Authors: Seong, Yeon-Sun, Kamijo, Keiju, Lee, Jae-Seon, Fernandez, Ester, Kuriyama, Ryoko, Miki, Toru, Lee, Kyung S
Format: Article
Language:English
Subjects:
Anaphase
Bone Neoplasms - genetics
Cell Cycle - genetics
Cell Cycle - physiology
Cell Cycle Proteins
Cell Division
Chromosome Aberrations
Humans
Mitosis
Osteosarcoma - genetics
Polo-Like Kinase 1
Prophase
Protein Kinases - chemistry
Protein Kinases - genetics
Protein Kinases - metabolism
Protein Serine-Threonine Kinases
Proto-Oncogene Proteins
Spindle Apparatus - physiology
Tumor Cells, Cultured
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Summary:Polo kinases play critical roles for proper M-phase progression. They are characterized by the presence of two regions of homology in the C-terminal non-catalytic domain, termed polo-box 1 (PB1) and polo-box 2 (PB2). Here we demonstrate that both PB1 and PB2 are required for targeting the catalytic activity of Plk1 to centrosomes, midbody, and kinetochores. Expression of either kinase-inactive PLK1/K82M or the C-terminal plk1 Δ N induced a pre-anaphase arrest with elevated Cdc2 and Plk1 activity. Prophase-arrested cells exhibited randomly oriented spindle structures, whereas metaphase cells exhibited aberrant bipolar spindles with Mad2 localization at kinetochores of misaligned chromosomes. Microtubule nucleation activity of centrosomes was not compromised. In vivo time-lapse studies revealed that expression of plk1 Δ N resulted in repeated cycles of bipolar spindle formation and disruption, suggestive of a defect in spindle stability. A prolonged arrest frequently led to the generation of micronucleated cells in the absence of sisterchromatid separation and centrosome duplication, indicating that micronucleation is not a result of accumulated cytokinesis failures. Interestingly, bypass of the mitotic arrest by dominant-negative spindle checkpoint components led to a failure in completion of cytokinesis. We propose that, in mammalian cells, the polo-box-dependent Plk1 activity is required for proper metaphase/anaphase transition and for cytokinesis.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M202602200