| Literature DB >> 17201418 |
Jeffrey J Rohde1, Marina A Pliushchev, Bryan K Sorensen, Dariusz Wodka, Qi Shuai, Jiahong Wang, Steven Fung, Katina M Monzon, William J Chiou, Liping Pan, Xiaoqing Deng, Linda E Chovan, Atul Ramaiya, Mark Mullally, Rodger F Henry, DeAnne F Stolarik, Hovis M Imade, Kennan C Marsh, David W A Beno, Thomas A Fey, Brian A Droz, Michael E Brune, Heidi S Camp, Hing L Sham, Ernst Uli Frevert, Peer B Jacobson, J T Link.
Abstract
Starting from a rapidly metabolized adamantane 11beta-hydroxysteroid dehydrogenase type 1 (11beta-HSD1) inhibitor 22a, a series of E-5-hydroxy-2-adamantamine inhibitors, exemplified by 22d and (+/-)-22f, was discovered. Many of these compounds are potent inhibitors of 11beta-HSD1 and are selective over 11beta-HSD2 for multiple species (human, mouse, and rat), unlike other reported species-selective series. These compounds have good cellular potency and improved microsomal stability. Pharmacokinetic profiling in rodents indicated moderate to large volumes of distribution, short half-lives, and a pharmacokinetic species difference with the greatest exposure measured in rat with 22d. One hour postdose liver, adipose, and brain tissue 11beta-HSD1 inhibition was confirmed with (+/-)-22f in a murine ex vivo assay. Although 5,7-disubstitued-2-adamantamines provided greater stability, a single, E-5-position, polar functional group afforded inhibitors with the best combination of stability, potency, and selectivity. These results indicate that adamantane metabolic stabilization sufficient to obtain short-acting, potent, and selective 11beta-HSD1 inhibitors has been discovered.Entities:
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Year: 2007 PMID: 17201418 DOI: 10.1021/jm0609364
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446