Esketamine inhaled as dry powder: Pharmacokinetic, pharmacodynamic and safety assessment in a preclinical study

Mikołaj Matłoka; Sylwia Janowska; Anna Gajos-Draus; Hubert Ziółkowski; Monika Janicka; Przemysław Perko; Kisło Kamil; Piotr Pankiewicz; Rafał Moszczyński-Pętkowski; Mateusz Mach; Paulina Dera; Krzysztof Abramski; Małgorzata Teska-Kamińska; Ewa Tratkiewicz; Maciej Wieczorek; Jerzy Pieczykolan

doi:10.1016/j.pupt.2022.102127

Esketamine inhaled as dry powder: Pharmacokinetic, pharmacodynamic and safety assessment in a preclinical study

Pulm Pharmacol Ther. 2022 Jun:73-74:102127. doi: 10.1016/j.pupt.2022.102127. Epub 2022 Apr 14.

Authors

Mikołaj Matłoka¹, Sylwia Janowska², Anna Gajos-Draus², Hubert Ziółkowski³, Monika Janicka², Przemysław Perko², Kisło Kamil², Piotr Pankiewicz², Rafał Moszczyński-Pętkowski², Mateusz Mach², Paulina Dera², Krzysztof Abramski², Małgorzata Teska-Kamińska², Ewa Tratkiewicz², Maciej Wieczorek², Jerzy Pieczykolan²

Affiliations

¹ R&D Centre, Celon Pharma SA, Marymoncka 15, 05-152, Kazun Nowy, Poland. Electronic address: mikolaj.matloka@celonpharma.com.
² R&D Centre, Celon Pharma SA, Marymoncka 15, 05-152, Kazun Nowy, Poland.
³ Department of Pharmacology and Toxicology, Faculty of Veterinary Medicine, University of Warmia and Mazury, Oczapowskiego 13, 10-718, Olsztyn, Poland.

PMID: 35429651
DOI: 10.1016/j.pupt.2022.102127

Abstract

Ketamine and its enantiomer esketamine have gained much attention in recent years as potent, fast-acting agents for the management of treatment-resistant depression. However, an alternative to oral ketamine administration is required to ensure adequate systemic exposure as the drug undergoes extensive first-pass metabolism. We propose dry powder inhalation as a new esketamine delivery route. Here, we examine the pharmacokinetics, pharmacodynamics, toxicology and safety of this novel esketamine administration method. Esketamine (10 mg/kg) and ketamine racemate (20 mg/kg) were administered to rats by dry powder inhalation, intravenous injection or intratracheal instillation and the pharmacokinetics of these treatments were compared. Analyte concentration of ketamine stereoisomers and their metabolites was assessed by LC-MS/MS method. Esketamine showed a clinically relevant pharmacokinetic profile, with high bioavailability (62%) and relatively low maximum concentration peaks. Esketamine exhibited high penetration of the blood-brain barrier, but pharmacodynamic examinations of brain homogenates showed no changes in selected protein phosphorylation or expression analyzed by the immunoblotting method. We conducted GLP-compliant 14-day and 28-day general toxicity studies in rats and dogs, respectively, subjected to dry esketamine powder inhalation. The maximum daily dosages were 46.5 mg/kg and 36.5 mg/kg, respectively. We also performed pharmacological safety studies. Esketamine inhaled as dry powder had an expected safety profile consistent with its known pharmacological action. None of its observed effects were considered toxicologically significant. The pharmacological safety studies confirmed that the observed effects were transient and that inhaled esketamine had a good safety profile. Hence, our preclinical studies demonstrated that dry powder inhalation is a highly efficacious and safe delivery route for esketamine and may be a viable alternative administration route meriting further clinical development.

Keywords: Antidepressant; Dry powder inhalation; Esketamine; Pharmacokinetics; Preclinical development; Toxicology&safety.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antidepressive Agents / pharmacology
Antidepressive Agents / therapeutic use
Chromatography, Liquid
Dogs
Ketamine* / adverse effects
Powders
Rats
Tandem Mass Spectrometry

Substances

Antidepressive Agents
Powders
Esketamine
Ketamine