| Literature DB >> 19522463 |
Martin R Tremblay1, André Lescarbeau, Michael J Grogan, Eddy Tan, Grace Lin, Brian C Austad, Lin-Chen Yu, Mark L Behnke, Somarajan J Nair, Margit Hagel, Kerry White, James Conley, Joseph D Manna, Teresa M Alvarez-Diez, Jennifer Hoyt, Caroline N Woodward, Jens R Sydor, Melissa Pink, John MacDougall, Matthew J Campbell, Jill Cushing, Jeanne Ferguson, Michael S Curtis, Karen McGovern, Margaret A Read, Vito J Palombella, Julian Adams, Alfredo C Castro.
Abstract
Recent evidence suggests that blocking aberrant hedgehog pathway signaling may be a promising therapeutic strategy for the treatment of several types of cancer. Cyclopamine, a plant Veratrum alkaloid, is a natural product antagonist of the hedgehog pathway. In a previous report, a seven-membered D-ring semisynthetic analogue of cyclopamine, IPI-269609 (2), was shown to have greater acid stability and better aqueous solubility compared to cyclopamine. Further modifications of the A-ring system generated three series of analogues with improved potency and/or solubility. Lead compounds from each series were characterized in vitro and evaluated in vivo for biological activity and pharmacokinetic properties. These studies led to the discovery of IPI-926 (compound 28), a novel semisynthetic cyclopamine analogue with substantially improved pharmaceutical properties and potency and a favorable pharmacokinetic profile relative to cyclopamine and compound 2. As a result, complete tumor regression was observed in a Hh-dependent medulloblastoma allograft model after daily oral administration of 40 mg/kg of compound 28.Entities:
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Year: 2009 PMID: 19522463 DOI: 10.1021/jm900305z
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446