S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine

Ketamine is a versatile drug used for many indications and is administered via various routes. Here, we report on the pharmacodynamics of sublingual and buccal fast-dissolving oral-thin-films that contain 50 mg of S-ketamine in a population of healthy male and female volunteers. Twenty volunteers re...

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Autores principales: Simons, Pieter, Olofsen, Erik, van Velzen, Monique, van Lemmen, Maarten, van Dasselaar, Tom, Mohr, Patrick, Hammes, Florian, van der Schrier, Rutger, Niesters, Marieke, Dahan, Albert
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pain Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9402896/
https://www.ncbi.nlm.nih.gov/pubmed/36034750
http://dx.doi.org/10.3389/fpain.2022.946487
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author Simons, Pieter
Olofsen, Erik
van Velzen, Monique
van Lemmen, Maarten
van Dasselaar, Tom
Mohr, Patrick
Hammes, Florian
van der Schrier, Rutger
Niesters, Marieke
Dahan, Albert
author_facet Simons, Pieter
Olofsen, Erik
van Velzen, Monique
van Lemmen, Maarten
van Dasselaar, Tom
Mohr, Patrick
Hammes, Florian
van der Schrier, Rutger
Niesters, Marieke
Dahan, Albert
author_sort Simons, Pieter
collection PubMed
description Ketamine is a versatile drug used for many indications and is administered via various routes. Here, we report on the pharmacodynamics of sublingual and buccal fast-dissolving oral-thin-films that contain 50 mg of S-ketamine in a population of healthy male and female volunteers. Twenty volunteers received one or two 50 mg S-ketamine oral thin films in a crossover design, placed for 10 min sublingually (n = 15) or buccally (n = 5). The following measurements were made for 6 h following the film placement: antinociception using three distinct pain assay; electrical, pressure, and heat pain, and drug high on an 11-point visual analog scale. Blood samples were obtained for the measurement of plasma S-ketamine, S-norketamine, and S-hydroxynorketamine concentrations. A population pharmacodynamic analysis was performed in NONMEM to construct a pharmacodynamic model of S-ketamine and its metabolites. P-values < 0.01 were considered significant. The sublingual and buccal 50 and 100 mg S-ketamine oral thin films were antinociceptive and produced drug high with effects lasting 2–6 h, although a clear dose-response relationship for antinociception could not be established. The effects were solely related to the parent compound with no contribution from S-norketamine or S-hydroxynorketamine. S-ketamine potency was lower for antinociception (C(50) ranging from 1.2 to 1.7 nmol/mL) than for drug high (C(50) 0.3 nmol/ml). The onset/offset of effect as defined by the blood-effect-site equilibration half-life did not differ among endpoints and ranged from 0 to 5 min. In conclusion, the 50-mg S-ketamine oral thin film was safe and produced long-term antinociception in all three nociceptive assays with side effects inherent to the use of ketamine. The study was registered at the trial register of the Dutch Cochrane Center (www.trialregister.nl) under identifier NL9267 and the European Union Drug Regulating Authorities Clinical Trials (EudraCT) database under number 2020-005185-33.
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spelling pubmed-94028962022-08-26 S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine Simons, Pieter Olofsen, Erik van Velzen, Monique van Lemmen, Maarten van Dasselaar, Tom Mohr, Patrick Hammes, Florian van der Schrier, Rutger Niesters, Marieke Dahan, Albert Front Pain Res (Lausanne) Pain Research Ketamine is a versatile drug used for many indications and is administered via various routes. Here, we report on the pharmacodynamics of sublingual and buccal fast-dissolving oral-thin-films that contain 50 mg of S-ketamine in a population of healthy male and female volunteers. Twenty volunteers received one or two 50 mg S-ketamine oral thin films in a crossover design, placed for 10 min sublingually (n = 15) or buccally (n = 5). The following measurements were made for 6 h following the film placement: antinociception using three distinct pain assay; electrical, pressure, and heat pain, and drug high on an 11-point visual analog scale. Blood samples were obtained for the measurement of plasma S-ketamine, S-norketamine, and S-hydroxynorketamine concentrations. A population pharmacodynamic analysis was performed in NONMEM to construct a pharmacodynamic model of S-ketamine and its metabolites. P-values < 0.01 were considered significant. The sublingual and buccal 50 and 100 mg S-ketamine oral thin films were antinociceptive and produced drug high with effects lasting 2–6 h, although a clear dose-response relationship for antinociception could not be established. The effects were solely related to the parent compound with no contribution from S-norketamine or S-hydroxynorketamine. S-ketamine potency was lower for antinociception (C(50) ranging from 1.2 to 1.7 nmol/mL) than for drug high (C(50) 0.3 nmol/ml). The onset/offset of effect as defined by the blood-effect-site equilibration half-life did not differ among endpoints and ranged from 0 to 5 min. In conclusion, the 50-mg S-ketamine oral thin film was safe and produced long-term antinociception in all three nociceptive assays with side effects inherent to the use of ketamine. The study was registered at the trial register of the Dutch Cochrane Center (www.trialregister.nl) under identifier NL9267 and the European Union Drug Regulating Authorities Clinical Trials (EudraCT) database under number 2020-005185-33. Frontiers Media S.A. 2022-08-11 /pmc/articles/PMC9402896/ /pubmed/36034750 http://dx.doi.org/10.3389/fpain.2022.946487 Text en Copyright © 2022 Simons, Olofsen, van Velzen, van Lemmen, van Dasselaar, Mohr, Hammes, van der Schrier, Niesters and Dahan. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pain Research
Simons, Pieter
Olofsen, Erik
van Velzen, Monique
van Lemmen, Maarten
van Dasselaar, Tom
Mohr, Patrick
Hammes, Florian
van der Schrier, Rutger
Niesters, Marieke
Dahan, Albert
S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title_full S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title_fullStr S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title_full_unstemmed S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title_short S-Ketamine oral thin film—Part 2: Population pharmacodynamics of S-ketamine, S-norketamine and S-hydroxynorketamine
title_sort s-ketamine oral thin film—part 2: population pharmacodynamics of s-ketamine, s-norketamine and s-hydroxynorketamine
topic Pain Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9402896/
https://www.ncbi.nlm.nih.gov/pubmed/36034750
http://dx.doi.org/10.3389/fpain.2022.946487
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