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Centrosome-associated Chk1 prevents premature activation of cyclin-B-Cdk1 kinase
A Kramer, N Mailand, C Lukas, RG Syljuasen, CJ Wilkinson, EA Nigg, J Bartek, J Lukas
Jazyk angličtina Země Anglie, Velká Británie
NLK
ProQuest Central
od 2000-01-01 do Před 1 rokem
Medline Complete (EBSCOhost)
od 1999-05-01 do 2015-11-30
Health & Medicine (ProQuest)
od 2000-01-01 do Před 1 rokem
PubMed
15311285
Knihovny.cz E-zdroje
- MeSH
- aktivace enzymů MeSH
- aparát dělícího vřeténka MeSH
- buněčné dělení MeSH
- buněčné linie MeSH
- centrozom * enzymologie MeSH
- cyklin B metabolismus MeSH
- cyklin B1 MeSH
- cykliny * metabolismus MeSH
- fosfatasy cdc25 fyziologie MeSH
- interfáze MeSH
- konfokální mikroskopie MeSH
- lidé MeSH
- proteinkinasa CDC2 fyziologie metabolismus MeSH
- proteinkinasy fyziologie metabolismus MeSH
- proteiny buněčného cyklu fyziologie MeSH
- vazba proteinů MeSH
- Check Tag
- lidé MeSH
Entry into mitosis occurs after activation of Cdk1, resulting in chromosome condensation in the nucleus and centrosome separation, as well as increased microtubule nucleation activity in the cytoplasm. The active cyclin-B1-Cdk1 complex first appears at the centrosome, suggesting that the centrosome may facilitate the activation of mitotic regulators required for the commitment of cells to mitosis. However, the signalling pathways involved in controlling the initial activation of Cdk1 at the centrosome remain largely unknown. Here, we show that human Chk1 kinase localizes to interphase, but not mitotic, centrosomes. Chemical inhibition of Chk1 resulted in premature centrosome separation and activation of centrosome-associated Cdk1. Forced immobilization of kinase-inactive Chk1 to centrosomes also resulted in premature Cdk1 activation. Conversely, under such conditions wild-type Chk1 impaired activation of centrosome-associated Cdk1, thereby resulting in DNA endoreplication and centrosome amplification. Activation of centrosomal Cdk1 in late prophase seemed to be mediated by cytoplasmic Cdc25B, whose activity is controlled by centrosome-associated Chk1. These results suggest that centrosome-associated Chk1 shields centrosomal Cdk1 from unscheduled activation by cytoplasmic Cdc25B, thereby contributing to proper timing of the initial steps of cell division, including mitotic spindle formation.
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- $a Entry into mitosis occurs after activation of Cdk1, resulting in chromosome condensation in the nucleus and centrosome separation, as well as increased microtubule nucleation activity in the cytoplasm. The active cyclin-B1-Cdk1 complex first appears at the centrosome, suggesting that the centrosome may facilitate the activation of mitotic regulators required for the commitment of cells to mitosis. However, the signalling pathways involved in controlling the initial activation of Cdk1 at the centrosome remain largely unknown. Here, we show that human Chk1 kinase localizes to interphase, but not mitotic, centrosomes. Chemical inhibition of Chk1 resulted in premature centrosome separation and activation of centrosome-associated Cdk1. Forced immobilization of kinase-inactive Chk1 to centrosomes also resulted in premature Cdk1 activation. Conversely, under such conditions wild-type Chk1 impaired activation of centrosome-associated Cdk1, thereby resulting in DNA endoreplication and centrosome amplification. Activation of centrosomal Cdk1 in late prophase seemed to be mediated by cytoplasmic Cdc25B, whose activity is controlled by centrosome-associated Chk1. These results suggest that centrosome-associated Chk1 shields centrosomal Cdk1 from unscheduled activation by cytoplasmic Cdc25B, thereby contributing to proper timing of the initial steps of cell division, including mitotic spindle formation.
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