Title of article
1H-Pyrazolo[3,4-g]hexahydro-isoquinolines as selective glucocorticoid receptor antagonists with high functional activity
Author/Authors
Robin D. Clark، نويسنده , , Nicholas C. Ray، نويسنده , , Karen Williams، نويسنده , , Paul Blaney، نويسنده , , Stuart Ward، نويسنده , , Peter H. Crackett، نويسنده , , Christopher Hurley، نويسنده , , Hazel J. Dyke، نويسنده , , David E. Clark، نويسنده , , Peter Lockey، نويسنده , , René Devos، نويسنده , , Melanie Wong، نويسنده , , Soraya S. Porres، نويسنده , , Colin P. Bright، نويسنده , , Robert E. Jenkins، نويسنده , , Joseph Belanoff، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2008
Pages
6
From page
1312
To page
1317
Abstract
Addition of the 4-fluorophenylpyrazole group to the previously described 2-azadecalin glucocorticoid receptor (GR) antagonist 1 resulted in significantly enhanced functional activity. SAR of the bridgehead substituent indicated that whereas groups as small as methyl afforded high GR binding, GR functional activity was enhanced by larger groups such as benzyl, substituted ethers, and aminoalkyl derivatives. GR antagonists with binding and functional activity comparable to mifepristone were discovered (e.g., 52: GR binding Ki 0.7 nM; GR reporter gene functional Ki 0.6 nM) and found to be highly selective over other steroid receptors. Analogues 43 and 45 had >50% oral bioavailability in the dog.
Keywords
Glucocorticoid receptor (GR) antagonist , Pyrazolo-fused azadecalins
Journal title
Bioorganic & Medicinal Chemistry Letters
Serial Year
2008
Journal title
Bioorganic & Medicinal Chemistry Letters
Record number
799158
Link To Document