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A Route to Potent, Selective, and Biased Salvinorin Chemical Space

Sarah J. Hill, Nathan Dao, Vương Đặng Quốc, Edward L. Stahl, Laura Bohn, Ryan A. Shenvi

2023ACS Central Science27 citationsDOIOpen Access PDF

Abstract

The salvinorins serve as templates for next generation analgesics, antipruritics, and dissociative hallucinogens via selective and potent agonism of the kappa-opioid receptor (KOR). In contrast to most opioids, the salvinorins lack basic amines and bind with high affinity and selectivity via complex polyoxygenated scaffolds that have frustrated deep-seated modification by synthesis. Here we describe a short asymmetric synthesis that relies on a sterically confined organocatalyst to dissociate acidity from reactivity and effect Robinson annulation of an unactivated nucleophile/unstable electrophile pair. Combined with a cobalt-catalyzed polarized diene-alkyne cycloaddition, the route allows divergent access to a focused library of salvinorins. We appraise the synthesis by its generation of multiple analogs that exceed the potency, selectivity, stability, and functional bias of salvinorin A itself.

Topics & Concepts

ChemistrySteric effectsCombinatorial chemistryChemical spaceSelectivityNucleophileCycloadditionStereochemistryAlkyneDrug discoveryOrganic chemistryCatalysisBiochemistryAlkaloids: synthesis and pharmacologyAsymmetric Synthesis and CatalysisChemical synthesis and alkaloids
A Route to Potent, Selective, and Biased Salvinorin Chemical Space | Litcius