Selective and potent agonists for estrogen receptor beta derived from molecular refinements of salicylaldoximes

被引:26
|
作者
Bertini, Simone [1 ]
De Cupertinis, Andrea [1 ]
Granchi, Carlotta [1 ]
Bargagli, Barbara [1 ]
Tuccinardi, Tiziano [1 ]
Martinelli, Adriano [1 ]
Macchia, Marco [1 ]
Gunther, Jillian R. [2 ]
Carlson, Kathryn E. [2 ]
Katzenellenbogen, John A. [2 ]
Minutolo, Filippo [1 ]
机构
[1] Univ Pisa, Dipartimento Sci Farmaceut, I-56126 Pisa, Italy
[2] Univ Illinois, Dept Chem, Urbana, IL 61801 USA
关键词
Estrogen; Receptor binding; Agonists; Salicylaldoxime; Docking; ER-BETA; DYNAMICS SIMULATION; BINDING-AFFINITY; LIGANDS; ALPHA; ANTIESTROGENS; TRANSCRIPTION; PROSTATE; MODELS; YANG;
D O I
10.1016/j.ejmech.2011.03.030
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
In a continuing effort to improve the subtype selectivity and agonist potency of estrogen receptor beta (ER beta) ligands, we have designed and developed a thus far unexplored structural series obtained by molecular refinements of monoaryl-substituted salicylaldoximes (Salaldox B). The most interesting compounds in this series (2c, d) show remarkably high ER beta-binding affinities, with K-i values reaching the sub-nanomolar range (K-i = 0.38 nM for 2c and 0.57 nM for 2d), and have very high levels of ER beta-subtype selectivity. Both compounds show a potent full agonist character on ER beta (EC50 = 0.23 nM for 2c and 1.3 nM for 2d). Furthermore, 2d shows a remarkable functional subtype selectivity, with a beta/alpha transcription potency ratio 50-fold higher than that of estradiol. (C) 2011 Elsevier Masson SAS. All rights reserved.
引用
收藏
页码:2453 / 2462
页数:10
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