A Review of the Metabolism and Relevance to Form and Formulation of Ketamine

P. Chue; A. Andreiev; J. Chue; J. Chue; M. Tate

doi:10.1192/j.eurpsy.2023.1783

European Psychiatry (Mar 2023)

A Review of the Metabolism and Relevance to Form and Formulation of Ketamine

P. Chue,
A. Andreiev,
J. Chue,
J. Chue,
M. Tate

Affiliations

P. Chue: University of Alberta, Edmonton
A. Andreiev: University of Ottawa, Ottawa
J. Chue: Oakville Trafalgar Memorial Hospital, Toronto
J. Chue: Amygdala Associates, Edmonton, Canada
M. Tate: Amygdala Associates, Edmonton, Canada

DOI: https://doi.org/10.1192/j.eurpsy.2023.1783
Journal volume & issue: Vol. 66
pp. S842 – S842

Abstract

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Introduction Ketamine is a phenylcyclohexylamine derivative comprising a racemic mixture of S- and R-ketamine that possesses anesthetic, analgesic, anti-inflammatory, and antidepressant activity. Oral (including extended release [PO]), intravenous (IV) sublingual (SL), transmucosal (TM), intranasal (IN), intramuscular (IM), rectal (PR), and subcutaneous (SC) formulations have been developed since its commercialization in 1970. Objectives To review and understand the impact of different forms and formulations on the pharmacokinetics of ketamine. Methods The extant literature on ketamine metabolism and formulations was reviewed and discussed. Results IV (racemic) ketamine (KET) has been shown to improve depressed mood within 4 hours with maximal effect at 24 hours. KET is a chiral molecule with two optimal isomers, R- and S-KET. KET is stereoselectively metabolized by CYP2B6 and CYP3A4 initially via nitrogen demethylation to active metabolite, norketamine (NK); there is no interconversion between R- and S-KET. NK is further metabolized to hydroxynorketamine (HNK) by CYP3A4 and CYP3A5; and dehydronorketamine (DHNK) by CYP2B6. Additional metabolic pathways exist including a direct enantioselective hydroxylation of KET to 6-hydroxyketamine (HK). Bioavailablity is greatest (100%) with the IV racemic KET formulation, but as low as 8% for oral S-KET due to extensive first-pass metabolism; the KET: NK ratio is a measure of first pass metabolism. NK plasma levels are higher with oral S-KET than KET as a result of local intestinal metabolism effects. Additionally, greater plasma concentrations are noted with IV bolus doses of S-KET vs. racemic KET or R-KET. S-KET possesses a longer elimination half-life than racemic KET due to inhibition by R-KET. KET is primarily renally eliminated and twice as fast in children vs. adults. Conclusions Complex interactions are reported between ketamine form (racemic/enantiomer), formulation, dose, and route of administration that impact on clinical variables and thus, outcome. Disclosure of Interest None Declared

Published in European Psychiatry

ISSN: 0924-9338 (Print); 1778-3585 (Online)
Publisher: Cambridge University Press
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system: Psychiatry
Website: https://www.cambridge.org/core/journals/european-psychiatry

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