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Fluoroalkylation of Dextromethorphan Improves CNS Exposure and Metabolic Stability

Jacob P. Sorrentino, Ryan A. Altman

2022ACS Medicinal Chemistry Letters21 citationsDOIOpen Access PDF

Abstract

Aryl-methyl ethers, while present in many bioactive compounds, are subject to rapid O-dealkylation, which can generate bioinactive or toxic metabolites. Such is the case for dextromethorphan, which readily undergoes P450 mediated O-dealkylation to provide the psychoactive phenolic metabolite dextrorphan, an N-methyl-d-aspartate (NMDA) receptor antagonist that causes hallucinations and encourages recreational abuse. As a general strategy to minimize this undesired degradation, both deuteration and fluorination strategies might be exploited, though such strategies have rarely been compared in matched series. In this manuscript, we designed, synthesized, and evaluated in vitro and in vivo new fluoroalkyl analogs of dextromethorphan and D3-dextromethorphan that minimize metabolic degradation and increased CNS exposure relative to dextromethorphan and related deuterated analogs currently in clinical trials.

Topics & Concepts

DextromethorphanDextrorphanMetaboliteNMDA receptorPharmacologyChemistryMetabolic stabilityIn vivoPhencyclidineAntagonistIn vitroReceptorMedicineBiochemistryBiologyBiotechnologyChemical Reactions and IsotopesFluorine in Organic ChemistryChemical Synthesis and Analysis