An efficient steroid pharmacophore-based strategy to identify new aromatase inhibitors

Aromatase, an enzyme involved in the conversion of androgens into estrogens, is an important target for the endocrine treatment of breast cancer. Aromatase inhibition is usually achieved with steroids structurally related to the substrate of catalysis or, alternatively, with azole non-steroid compou...

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Veröffentlicht in:European journal of medicinal chemistry 2009-10, Vol.44 (10), p.4121-4127
Hauptverfasser: Neves, Marco A.C., Dinis, Teresa C.P., Colombo, Giorgio, Sá e Melo, M. Luisa
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Sprache:eng
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Zusammenfassung:Aromatase, an enzyme involved in the conversion of androgens into estrogens, is an important target for the endocrine treatment of breast cancer. Aromatase inhibition is usually achieved with steroids structurally related to the substrate of catalysis or, alternatively, with azole non-steroid compounds. Substituted androstenedione derivatives with Δ 1, Δ 6 and Δ 1,6 unsaturations and 6-alkyl/6-phenyl aliphatic substitutions, are among the most potent steroid aromatase inhibitors known to date. In this paper we have combined the common pharmacophoric and shape features of these molecules into a new pharmacophore model, useful for virtual screening of large compound databases. Small subsets of the best fitting anti-aromatase candidates were extracted from the NCI database and experimentally tested on an in vitro assay with human placental aromatase. New potent aromatase inhibitors were identified such as compounds 8 and 14. Considering the lack of a crystal structure for the aromatase enzyme, this ligand-based method is a valuable tool for the virtual screening of new aromatase inhibitors. New potent aromatase inhibitors were identified on the NCI database using a fast and efficient virtual screening strategy based on a pharmacophore model derived from C6-substituted androstenedione derivatives. [Display omitted]
ISSN:0223-5234
1768-3254
DOI:10.1016/j.ejmech.2009.05.003