Literature DB >> 11262093

Syntheses and biological activities of a novel group of steroidal derived inhibitors for human Cdc25A protein phosphatase.

H Peng1, W Xie, D M Otterness, J P Cogswell, R T McConnell, H L Carter, G Powis, R T Abraham, L H Zalkow.   

Abstract

Silica gel supported pyrolysis of an azido-homo-oxa steroid led to rearrangement, presumably by a mechanism similar to that of solution phase Schmidt fragmentation, to produce a group of novel inhibitors for the oncogenic cell cycle regulator Cdc25A phosphatase. Cyano-containing acid 17, one of the best inhibitors in this group, inhibited the activity of Cdc25A protein phosphatase reversibly and noncompetitively with an IC(50) value of 2.2 microM. Structure-activity relationships revealed that a phosphate surrogate such as a carboxyl or a xanthate group is required for inhibitory activity, and a hydrophobic alkyl chain, such as the cholesteryl side chain, contributes greatly to the potency. Without the cyano group, acid 26 and xanthate 27 were found to be more selective over Cdc25A (IC(50) = 5.1 microM and 1.1 microM, respectively) than toward CD45 (IC(50) > 100 microM, in each case), a receptor protein tyrosine phosphatase. Several of these inhibitors showed antiproliferative activities in the NCI 60-human tumor cell line screen. These steroidal derived Cdc25 inhibitors provide unique leads for the development of dual-specificity protein phosphatase inhibitors.

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Year:  2001        PMID: 11262093     DOI: 10.1021/jm0004401

Source DB:  PubMed          Journal:  J Med Chem        ISSN: 0022-2623            Impact factor:   7.446


  5 in total

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Review 4.  Is Cdc25 a druggable target?

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Journal:  Anticancer Agents Med Chem       Date:  2008-12       Impact factor: 2.505

Review 5.  Mechanism targeted discovery of antitumor marine natural products.

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Journal:  Curr Med Chem       Date:  2004-07       Impact factor: 4.530

  5 in total

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