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Optimization of purine based PDE1/PDE5 inhibitors to a potent and selective PDE5 inhibitor for the treatment of male ED
Authors:Boyle Craig D  Xu Ruo  Asberom Theodros  Chackalamannil Samuel  Clader John W  Greenlee William J  Guzik Henry  Hu Yuequing  Hu Zhiyong  Lankin Claire M  Pissarnitski Dmitri A  Stamford Andrew W  Wang Yuguang  Skell Jeffrey  Kurowski Stanley  Vemulapalli Subbarao  Palamanda Jairam  Chintala Madhu  Wu Ping  Myers Joyce  Wang Peng
Affiliation:Schering-Plough Research Institute, 2015 Galloping Hill Road, Kenilworth, NJ 07033, USA. craig.boyle@spcorp.com
Abstract:In search of a PDE5 inhibitor for erectile dysfunction, an SAR was developed from a PDE1/PDE5 purine series of leads, which had modest PDE5 potency and poor isozyme selectivity. A compound (41) with PDE5 inhibition and in vivo activity similar to sildenafil was discovered from this effort. In addition, purine 41 demonstrated superior overall PDE isozyme selectivity when compared to the approved PDE5 inhibitors sildenafil, vardenafil, and tadalafil, which may result in a more favorable side-effect profile.
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