• Bioorg. Med. Chem. Lett. · Nov 2001

    Comparative Study

    Cantharimides: a new class of modified cantharidin analogues inhibiting protein phosphatases 1 and 2A.

    • A McCluskey, C Walkom, M C Bowyer, S P Ackland, E Gardiner, and J A Sakoff.
    • Medicinal Chemistry Group, School of Biological and Chemical Sciences, The University of Newcastle, Callaghan, NSW 2038, Australia. amcclusk@mail.newcastle.edu.au
    • Bioorg. Med. Chem. Lett. 2001 Nov 19; 11 (22): 2941-6.

    AbstractCantharidin and its analogues have been of considerable interest as potent inhibitors of the serine/threonine protein phosphatases 1 and 2A (PP1 and PP2A). However, limited modifications to the parent compounds is tolerated. As part of an on-going study we have developed a new series of cantharidin analogues, the cantharimides. Inhibition studies indicate that cantharimides possessing a D- or L-histidine, are more potent inhibitors of PP1 and PP2A (PP1 IC(50)=3.22+/-0.7 microM; PP2A IC(50)=0.81+/-0.1 microM and PP1 IC(50)=2.82+/-0.6 microM; PP2A IC(50)=1.35+/-0.3 microM, respectively) than norcantharidin (PP1 IC(50)=5.31+/-0.76 microM; PP2A IC(50)=2.9+/-1.04 microM) and essentially equipotent with cantharidin (PP1 IC(50)=3.6+/-0.42 microM; PP2A IC(50)=0.36+/-0.08 microM). Cantharimides with non-polar or acidic amino acid residues are only poor inhibitors of PP1 and PP2A.

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