Literature

Abstract

Modification of the C-1 ketone of salvinorin A (2a) produces analogues with opioid antagonist properties. Of particular significance is the finding that 1-deoxo-1,10-dehydrosalvinorin A (11a) is a moderately potent antagonist at all three opioid receptor subtypes, and that herkinorin (2b), a mu agonist, is converted to a weak antagonist by removal of the C-1 ketone (3b and 11b). These observations suggest that the ketone of 2b is a key structural feature responsible for mu agonist activity.

DOI： 10.1016/j.bmcl.2007.09.050

Synthetic studies of neoclerodane diterpenes from Salvia divinorum: Exploration of the 1-position

Bioorganic & Medicinal Chemistry Letters 2007.0

Synthetic Studies of Neoclerodane Diterpenes from Salvia divinorum: Preparation and Opioid Receptor Activity of Salvinicin Analogues

Journal of Medicinal Chemistry 2007.0

Synthetic Studies of Neoclerodane Diterpenes from Salvia divinorum: Semisynthesis of Salvinicins A and B and Other Chemical Transformations of Salvinorin A

Journal of Natural Products 2006.0

Neoclerodane Diterpenes as a Novel Scaffold for μ Opioid Receptor Ligands

Journal of Medicinal Chemistry 2005.0

Synthesis and κ-Opioid Receptor Activity of Furan-Substituted Salvinorin A Analogues

Journal of Medicinal Chemistry 2014.0

Synthetic studies of neoclerodane diterpenes from Salvia divinorum: Selective modification of the furan ring