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Your search keyword '"Mirella A. Keane"' showing total 5 results
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5 results on '"Mirella A. Keane"'

1. Anhydride modified cantharidin analogues. Is ring opening important in the inhibition of protein phosphatase 2A?

Author

Jennette A. Sakoff, Lisa-Maree Mudgee, Adam McCluskey, Alistair T. R. Sim, Ronald J. Quinn, and Mirella A. Keane

Subjects
Pharmacology, Cantharidin, Magnetic Resonance Spectroscopy, Molecular Structure, Stereochemistry, Organic Chemistry, General Medicine, Protein phosphatase 2, Ring (chemistry), Anhydrides, chemistry.chemical_compound, chemistry, Drug Discovery, Phosphoprotein Phosphatases, Moiety, Protein Phosphatase 2, Enzyme Inhibitors
Abstract

A series of anhydride modified cantharidin analogues have been synthesised and screened for their ability to inhibit protein phosphatase 2A. Surprisingly only analogues capable of undergoing a facile ring opening of the anhydride moiety displayed any significant inhibition. Subsequent NMR experiments indicated that 7-oxobicyclo[2.2.1]heptane-2,3-dicarboxylic acid was the major (sole) species under assay conditions. The ability of these modified anhydro-cantharidin analogues to inhibit protein phosphatase 2A varies from 4 (16) to 100% (8) at 100 μM test concentration.

Published
2000
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2. ChemInform Abstract: The First Two Cantharidin Analogues Displaying PP1 Selectivity

Author

Alistair T. R. Sim, Jennette A. Sakoff, Michael C. Bowyer, Adam McCluskey, David J. Young, Cecilia C. Walkom, and Mirella A. Keane

Subjects
chemistry.chemical_compound, Cantharidin, chemistry, Furan, High pressure, Thiophene, General Medicine, Selectivity, Thiophene derivatives, Maleimide, Medicinal chemistry
Abstract

High pressure Diels-Alder reactions of furan and dimethylmaleate, and thiophene and maleimide resulted in two cantharidin analogues, 3 and 6 possessing PP1 selectivity (>40- and >30-fold selectivity) over PP2A. Both compounds exhibited moderate PP1 activity, 3 IC 50 50 μM and 6 IC 50 12.5 μM. Interestingly, the corresponding mono-ester derivatives of 3 showed no such selectivity.

Published
2010
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3. Anticancer activity and protein phosphatase 1 and 2A inhibition of a new generation of cantharidin analogues

Author

Monique L. Baldwin, Adam McCluskey, Mirella A. Keane, Stephen P. Ackland, and Jennette A. Sakoff

Subjects
HL60, Antineoplastic Agents, Pharmacology, chemistry.chemical_compound, Structure-Activity Relationship, Protein Phosphatase 1, Phosphoprotein Phosphatases, Tumor Cells, Cultured, Humans, Pharmacology (medical), Fostriecin, Enzyme Inhibitors, Cantharidin, biology, Cell Cycle, Protein phosphatase 1, Biological activity, Protein phosphatase 2, DNA, Cell cycle, Oncology, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Drug Screening Assays, Antitumor
Abstract

Cantharidin (Spanish Fly) is a natural toxin and an inhibitor of protein phosphatases 1 (PP1) and 2A (PP2A), which have key roles in cell cycle progression. We have synthesised two series of demethylated cantharidin analogues, one displaying an open-ring lactone configuration in solution (Novo-1 to Novo-5) similar to cantharidin, the other showing a closed-ring lactone configuration (Novo-6 to Novo-10). In the present study, these ten agents were screened for in vitro PP1 and PP2A inhibition and cellular cytotoxicity in nine cancer cell lines of haematopoietic (L1210, HL60), ovarian (A2780, ADDP), osteo (143B), and colon (HCT116, HT29, WiDr, SW480) origin and one normal colon cell line (CCD-018). The open-ring series (IC50, PPI=2.0-4.8 microM, PP2A=0.2-0.5 microM) maintained the PP2A selectivity of cantharidin (IC50, PPI=1.8 microM, PP2A=0.2 microM), although some were less potent. The closed-ring series (IC50, PPI=12.5-1000 microM, PP2A=5-1000 microM) were considerably less potent inhibitors, confirming the need of ring opening for inhibition. The cytotoxicity (IC50, 72 h, MTT assay) of cantharidin ranged from 6-15 microM, while the new analogues ranged from 14 to1000 microM. Cytotoxicity of the agents did not consistently parallel the in vitro potency of protein phosphatase inhibition. A number of analogues showed colon cancer selectivity, particularly Novo-6, where the cytotoxicity ranged from 14-88 microM in the colon cancer cells and 275-680 microM in all other cell lines including normal colon cells. The reason for this selectivity was not apparent and may involve additional intracellular targets. Cell cycle analysis showed cantharidin to enhance cell cycle progression as evident from an increased S-phase population and enhanced DNA synthesis, culminating in G2/M arrest and apoptosis. With Novo-1 and Novo-6, the cell cycle changes paralleled the cytotoxicity responses, with the predominant effect of G2/M cell cycle arrest followed by cell death. In conclusion, we have synthesised new anticancer agents that show selective cytotoxicity in colon cancer cells while remaining inactive in normal colon cells, and which mediate their effects via the G2/M phase of the cell cycle.

Published
2002

4. The first two cantharidin analogues displaying PP1 selectivity

Author

Mirella A. Keane, Jennette A. Sakoff, Michael C. Bowyer, David J. Young, Adam McCluskey, Cecilia C. Walkom, and Alistair T. R. Sim

Subjects
Cantharidin, Bicyclic molecule, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Chemical synthesis, Substrate Specificity, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Furan, Drug Discovery, Thiophene, Phosphoprotein Phosphatases, Molecular Medicine, Indicators and Reagents, Enzyme Inhibitors, Selectivity, Imide, Molecular Biology, Maleimide
Abstract

High pressure Diels-Alder reactions of furan and dimethylmaleate, and thiophene and maleimide resulted in two cantharidin analogues, 3 and 6 possessing PP1 selectivity (>40- and >30-fold selectivity) over PP2A. Both compounds exhibited moderate PP1 activity, 3 IC 50 50 μM and 6 IC 50 12.5 μM. Interestingly, the corresponding mono-ester derivatives of 3 showed no such selectivity.

Published
2002

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