| Literature DB >> 30852901 |
Fernanda M F Roleira1,2, Carla Varela1,2, Cristina Amaral3, Saul C Costa1, Georgina Correia-da-Silva3, Federica Moraca4,5,6, Giosuè Costa4,6, Stefano Alcaro4,6, Natércia A A Teixeira3, Elisiário J Tavares da Silva1,2.
Abstract
C-6α and C-7α androstanes were studied to disclose which position among them is more convenient to functionalize to reach superior aromatase inhibition. In the first series, the study of C-6 versus C-7 methyl derivatives led to the very active compound 9 with IC50 of 0.06 μM and Ki = 0.025 μM (competitive inhibition). In the second series, the study of C-6 versus C-7 allyl derivatives led to the best aromatase inhibitor 13 of this work with IC50 of 0.055 μM and Ki = 0.0225 μM (irreversible inhibition). Beyond these findings, it was concluded that position C-6α is better to functionalize than C-7α, except when there is a C-4 substituent simultaneously. In addition, the methyl group was the best substituent, followed by the allyl group and next by the hydroxyl group. To rationalize the structure-activity relationship of the best inhibitor 13, molecular modeling studies were carried out.Entities:
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Year: 2019 PMID: 30852901 DOI: 10.1021/acs.jmedchem.9b00157
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446