|
|||||
|
|
Arylpropanolamines: selective beta3 agonists arising from strategies to mitigate phase I metabolic transformations |
|
| Authors: | Washburn W N Harper T W Wu G Godfrey J D McCann P Girotra R Shao C Zhang H Gavai A Mikkilineni A Dejneka T Ahmed S Caringal Y Hangeland J Zhang M Cheng P T W Russell A D Skwish S Slusarchyk D A Allen G T Frohlich B H Abboa-Offei B E Cap M Waldron T L George R J Tesfamariam B Dickinson K E Seymour A A Sher P M |
| Institution: | Bristol-Myers Squibb Pharmaceutical Research Institute, PO Box 4000, Princeton, NJ 08543, USA. William.Washburn@bms.com |
| Abstract: | Utilization of N-substituted-4-hydroxy-3-methylsulfonanilidoethanolamines 1 as selective beta(3) agonists is complicated by their propensity to undergo metabolic oxidative N-dealkylation, generating 0.01-2% of a very potent alpha(1) adrenergic agonist 2. A summary of the SAR for this hepatic microsomal conversion precedes presentation of strategies to maintain the advantages of chemotype 1 while mitigating the consequences of N-dealkylation. This effort led to the identification of 4-hydroxy-3-methylsulfonanilidopropanolamines 15 for which the SAR for the unique stereochemical requirements for binding to the beta adrenergic receptors culminated in the identification of the potent, selective beta(3) agonist 15f. |
| Keywords: | |
| 本文献已被 ScienceDirect PubMed 等数据库收录! | |