Synthesis of 6,14-epoxymorphinan derivatives and their pharmacologies

A novel 6,14-epoxymorphinan benzamide derivative (NS22) that was previously reported showed opioid κ receptor agonistic activity and analgesic activity. The unsatisfactory κ selectivity of NS22 led us to synthesize its derivatives to improve the opioid κ receptor selectivity and the agonist activity. In the course of SAR of the various derivatives, 17-benzyl-6,14-epoxymorphinan derivatives (KNT-33, 53, 55, 80, 90, 133) were found to show high selectivities and affinities for the opioid κ receptor. In addition, KNT-33, 53, 55 showed dose-dependent analgesic effects in acetic acid writhing tests. Therefore, 17-benzyl substituents may play an important role for developing κ selectivity.

We found that 17-benzyl-6,14-epoxymorphinan derivatives showed high selectivities for the opioid κ receptor. The 17-benzyl substituent may play an important role for developing κ selectivity.Figure optionsDownload as PowerPoint slide