Distinct regulators for Plk1 activation in starfish meiotic and early embryonic cycles

Okano-Uchida, Takayuki; Okumura, Eiichi; Iwashita, Motoko; Yoshida, Hitoshi; Tachibana, Kazunori; Kishimoto, Takeo

doi:10.1093/emboj/cdg535

Cited by 61 publications

(79 citation statements)

References 42 publications

(77 reference statements)

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“…Indeed, Plk1 can phosphorylate and thereby regulate both Cdc25C (12) and the Cdk1 inhibitor Myt1 (13,14). This would seem consistent with the hypothesis that Plk1 is the ''trigger'' kinase for the activation of Cdk1.…”

supporting

confidence: 57%

Molecular and structural basis of polo-like kinase 1 substrate recognition: Implications in centrosomal localization

García‐Álvarez

Cárcer

Ibañez

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

102

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Polo-like kinase (Plk1) is crucial for cell cycle progression through mitosis. Here we present the molecular and structural mechanisms that regulate the substrate recognition of Plk1 and influence its centrosomal localization and activity. Our work shows that Plk1 localization is controlled not only by the polo box domain (PBD); remarkably, the kinase domain is also involved in Plk1 targeting mechanism to the centrosome. The crystal structures of the PBD in complex with Cdc25C and Cdc25C-P target peptides reveal that Trp-414 is fundamental in their recognition regardless of its phosphorylation status. Binding measurements demonstrate that W414F mutation abolishes molecular recognition and diminishes centrosomal localization. Therefore, Plk1 centrosomal localization is not controlled by His-538 and Lys-540, the residues involved in phosphorylated target binding. The different conformations of the loop, which connects the polo boxes in the apo and the PBD-Cdc25C and PBD-Cdc25C-P complex structures, together with changes in the proline adjacent to the phosphothreonine in the target peptide, suggest a regulatory mechanism to detect binding of unphosphorylated or phosphorylated target substrates. Altogether, these data propose a model for the interaction between Plk1 and Cdc25C.cell cycle ͉ enzymes ͉ kinase ͉ protein structure ͉ polo box domain

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supporting

confidence: 57%

Molecular and structural basis of polo-like kinase 1 substrate recognition: Implications in centrosomal localization

García‐Álvarez

Cárcer

Ibañez

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

102

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“…It is involved in regulating multiple biological events in cancer cell proliferation [14]. In recent years, Plk1 has been discovered to also play regulatory roles in germ cells and oocytes, such as mouse [18], porcine [19], and starfish [20]. The recent focus of research has been on some Bexperimental or model^animals, such as Drosophila melanogaster [21], zebrafish [2], and mice [1].…”

Section: Discussionmentioning

confidence: 99%

Plk1 inhibition leads to a failure of mitotic division during the first mitotic division in pig embryos

Zhang

Chen

Cui

et al. 2017

J Assist Reprod Genet

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Purpose This study was conducted to examine the dynamic distribution of polo-like 1 kinase (Plk1) and the possible role it plays in first mitotic division during early porcine embryo development. Methods Indirect immunofluorescence and confocal microscopy imaging techniques combined with western blot analyses were used to study the dynamic expression and subcellular localization of Plk1 protein in pig parthenogenetic embryos. Finally, a selective Plk1 inhibitor, GSK461364, was used to evaluate the potential role of Plk1 during this special stage.Results The results showed that Plk1 upon expression exhibited specific dynamic intracellular localization, which closely correlated with the α-tubulin distribution during the first mitotic division. GSK461364 treatment resulted in cleavage failure, with majority of the GSK461364-treated embryos being arrested in prometaphase. Further results of the subcellular structure examination showed that GSK461364 treatment led to a significantly higher proportion of the treated embryos having abnormal spindles and misarranged chromosomes at the prometaphase stage. Conclusions Thus, these results indicated that Plk1 is essential for porcine embryos to complete the first mitotic division. Furthermore, Plk1 regulation was associated with effects on spindle assembly and chromosome arrangement.

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“…However, more recent studies (42,43) have shown that Plk1 is implicated in a positive feedback loop that consists of both Plk1 and CDK1, and it does not function as the initial activator, rather its activation depends upon CDK1 activity. Our study seems to shed new light on this controversial issue, as the inhibitory effect of olomoucine on Plk1-mediated B23 Ser-4 phosphorylation that we observed here strongly implies that the B23 phosphorylation activity of Plk1 during M-phase is dependent upon CDK1 activation.…”

Section: Discussionmentioning

confidence: 99%

B23/Nucleophosmin Serine 4 Phosphorylation Mediates Mitotic Functions of Polo-like Kinase 1

Zhang

Shi

Paddon

et al. 2004

Journal of Biological Chemistry

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Distinct regulators for Plk1 activation in starfish meiotic and early embryonic cycles

Cited by 61 publications

References 42 publications

Molecular and structural basis of polo-like kinase 1 substrate recognition: Implications in centrosomal localization

Molecular and structural basis of polo-like kinase 1 substrate recognition: Implications in centrosomal localization

Plk1 inhibition leads to a failure of mitotic division during the first mitotic division in pig embryos

B23/Nucleophosmin Serine 4 Phosphorylation Mediates Mitotic Functions of Polo-like Kinase 1

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