Two new competing pathways establish the threshold for cyclin-B–Cdk1 activation at the meiotic G2/M transition

Hiraoka, Daisaku; Aono, Ryota; Hanada, Shinichiro; Okumura, Eiichi; Kishimoto, Takeo

doi:10.1242/dev.143743

Cited by 6 publications

(7 citation statements)

References 42 publications

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“…Consistent with this, using U2OS cell line treated with DIA-001, we showed that PARP cleavage was enhanced. We also show that cyclin A levels increase after treatment with DIA-001 but cyclin B level increase only slightly suggesting cell cycle progression through the S/G2 transition but arrested at the G2/M phase (15)(16)(17). Together, the data from our study indicates that treatment with DIA-001 may induce cell cycle arrest in G2 phase and apoptosis in cancer cells.…”

Section: Discussionsupporting

confidence: 61%

A novel topoisomerase I inhibitor DIA-001 induces DNA damage mediated cell cycle arrest and apoptosis in cancer cell

et al. 2020

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Background: DNA topoisomerase enzyme plays an essential role in controlling the DNA topology structure by binding to DNA and cutting the phosphate backbone of either one or both of the DNA strands.Here, we have identified a small molecule inhibitor, DIA-001, that directly binds to Topoisomerase 1 (Topo I) and promotes the Topo I-DNA adducts. Methods: In this study, we investigated the antitumor effects of DIA-001 using MTS assay and colony formation. We examined cell cycle of tumor cells with DIA-001 treatment in vitro by flow cytometry. And we investigated DNA damage and cell cycle marker protein after treatment with DIA-001 at different concentration and time point by western blot. Immunofluorescence was performance to detect the nuclear foci. The effects of DIA-001 on Topo I and Topo II activities were examined by DNA relaxation assays. Results: We demonstrate that DIA-001 inhibit DNA replication and arrest cell cycle progression at the G2/M phase by directly binds to Topo I and promotes the Topo I-DNA adducts. In addition, DIA-001 can activate the DNA damage response signaling cascade, resulting in apoptosis in treated cells.Conclusions: Our findings show a novel compound for treatment of cancer cells with the potential as a chemotherapy candidate that is less toxic to normal cells.

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Section: Discussionsupporting

confidence: 61%

A novel topoisomerase I inhibitor DIA-001 induces DNA damage mediated cell cycle arrest and apoptosis in cancer cell

et al. 2020

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“…Hence, it seems that Plac1 knockdown affected both Akt and MPF activity. Of interest, in meiotic starfish oocytes, Akt directly phosphorylates both Cdc25 phosphatase and Myt1 kinase, which results in the activation of cyclin B-Cdk1 and meiosis resumption (40), further supporting to idea that the Akt pathway might the primary downstream signal of Plac1.…”

Section: Discussionmentioning

confidence: 72%

Placenta‐specific 1 regulates oocyte meiosis and fertilization through furin

Shi

Zhu

et al. 2018

FASEB j.

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Placenta-specific 1 (Plac1) has been found to be essential for placentation, and abnormal Plac1 expression and distribution is highly correlated with preeclampsia and implantation failure; however, its function in mammalian oocytes has not been elucidated. Here, we report that Plac1 was more prominent in mouse oocytes and enriched at the membrane region throughout meiosis. On the one hand, Plac1 knockdown severely disrupted microvillus organization; however, on the other hand, Plac1 significantly decreased oocyte maturation and increased aneuploidy, consequently disrupting normal fertilization. On the basis of immunoprecipitate matrix-assisted laser desorption/ionization, we established a working model, then verified and suggested that, at the germinal vesicle stage, Plac1 enriches the membrane to activate furin, and active furin subsequently activates IGF-1 receptor to maintain regular microvillus organization. Upon meiosis onset, active furin/IGF-1 receptor relocates into the cytoplasm to activate (phosphorylate) Akt to promote meiosis. In summary, our finding suggests that Plac1, a protein that is crucial for placentation, is also essential for oocyte meiosis and fertilization.-Shi, L.-Y., Ma, Y., Zhu, G.-Y., Liu, J.-W., Zhou, C.-X., Chen, L.-J., Wang, Y., Li, R.-C., Yang, Z.-X., Zhang, D. Placenta-specific 1 regulates oocyte meiosis and fertilization through furin.

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“…16 In vertebrate cells, the entry of MPF into the nucleus during prophase was thought to be essential for the induction and coordination of M-phase events. 30,31 During the mitosis, Akt may regulate the intracellular localization and activation of Cdc2 by phosphorylating Cdc25B. [32][33][34][35] In this study, we used SH-6, a specific inhibitor of pAkt1 (Ser473), to track the function of pAkt1 (Ser473) in the release of diplotene arrest of mouse oocytes.…”

Section: Discussionmentioning

confidence: 99%

Protein kinase Cδ (PKCδ) involved in the regulation of pAkt1 (Ser473) on the release of mouse oocytes from diplotene arrest

Liu

et al. 2018

Cell Biochemistry & Function

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As a drug target, Akt is still the focus of research in somatic and fertilized eggs. Here, our data depicted a series of molecular events of pAkt1 (Ser473) and PKCδ via their special inhibitor and antibody in order to analyse their role and relationship on the release of mouse oocytes from diplotene arrest. Our results may offer important data for clinic research scientist to recognize the target role of pAkt1 (Ser473) via PKCδ in cell cycle regulation.

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Two new competing pathways establish the threshold for cyclin-B–Cdk1 activation at the meiotic G2/M transition

Cited by 6 publications

References 42 publications

A novel topoisomerase I inhibitor DIA-001 induces DNA damage mediated cell cycle arrest and apoptosis in cancer cell

A novel topoisomerase I inhibitor DIA-001 induces DNA damage mediated cell cycle arrest and apoptosis in cancer cell

Placenta‐specific 1 regulates oocyte meiosis and fertilization through furin

Protein kinase Cδ (PKCδ) involved in the regulation of pAkt1 (Ser473) on the release of mouse oocytes from diplotene arrest

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