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Pharmacophore-guided discovery of CDC25 inhibitors causing cell cycle arrest and tumor regression

Articolo
Data di Pubblicazione:
2019
Abstract:
CDC25 phosphatases play a key role in cell cycle transitions and are important targets for cancer therapy. Here, we set out to discover novel CDC25 inhibitors. Using a combination of computational methods, we defined a minimal common pharmacophore in established CDC25 inhibitors and performed virtual screening of a proprietary library. Based on the availability of crystal structures for CDC25A and CDC25B, we implemented a molecular docking strategy and carried out hit expansion/optimization. Enzymatic assays revealed that naphthoquinone scaffolds were the most promising CDC25 inhibitors among selected hits. At the molecular level, the compounds acted through a mixed-type mechanism of inhibition of phosphatase activity, involving reversible oxidation of cysteine residues. In 2D cell cultures, the compounds caused arrest of the cell cycle at the G1/S or at the G2/M transition. Mitotic markers analysis and time-lapse microscopy confirmed that CDK1 activity was impaired and that mitotic arrest was followed by death. Finally, the compounds induced differentiation, accompanied by decreased stemness properties, in intestinal crypt stem cell-derived Apc/K-Ras-mutant mouse organoids, and led to tumor regression and reduction of metastatic potential in zebrafish embryo xenografts used as in vivo model.
Tipologia CRIS:
01.01 - Articolo in rivista
Keywords:
Multidisciplinary
Elenco autori:
Kabakci, Zeynep; Käppeli, Simon; Cantù, Claudio; Jensen, Lasse D.; König, Christiane; Toggweiler, Janine; Gentili, Christian; Ribaudo, Giovanni; Zagotto, Giuseppe; Basler, Konrad; Pinna, Lorenzo A.; Cozza, Giorgio; Ferrari, Stefano
Autori di Ateneo:
COZZA GIORGIO
PINNA LORENZO
ZAGOTTO GIUSEPPE
Link alla scheda completa:
https://www.research.unipd.it/handle/11577/3291299
Link al Full Text:
https://www.research.unipd.it//retrieve/handle/11577/3291299/353806/s41598-019-38579-7.pdf
Pubblicato in:
SCIENTIFIC REPORTS
Journal
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URL

www.nature.com/srep/index.html
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