Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study

BACKGROUND AND AIMS: Take‐home naloxone can prevent death from heroin/opioid overdose, but pre‐provision is difficult because naloxone is usually given by injection. Non‐injectable alternatives, including naloxone nasal sprays, are currently being developed. To be effective, the intranasal (i.n.) sp...

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Autores principales: McDonald, Rebecca, Lorch, Ulrike, Woodward, Jo, Bosse, Björn, Dooner, Helen, Mundin, Gill, Smith, Kevin, Strang, John
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Research Reports
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836974/
https://www.ncbi.nlm.nih.gov/pubmed/29143400
http://dx.doi.org/10.1111/add.14033
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author McDonald, Rebecca
Lorch, Ulrike
Woodward, Jo
Bosse, Björn
Dooner, Helen
Mundin, Gill
Smith, Kevin
Strang, John
author_facet McDonald, Rebecca
Lorch, Ulrike
Woodward, Jo
Bosse, Björn
Dooner, Helen
Mundin, Gill
Smith, Kevin
Strang, John
author_sort McDonald, Rebecca
collection PubMed
description BACKGROUND AND AIMS: Take‐home naloxone can prevent death from heroin/opioid overdose, but pre‐provision is difficult because naloxone is usually given by injection. Non‐injectable alternatives, including naloxone nasal sprays, are currently being developed. To be effective, the intranasal (i.n.) spray dose must be adequate but not excessive, and early absorption must be comparable to intramuscular (i.m.) injection. We report on the pharmacokinetics (PK) of a specially produced concentrated novel nasal spray. The specific aims were to: (1) estimate PK profiles of i.n. naloxone, (2) compare early systemic exposure with i.n. versus i.m. naloxone and (3) estimate i.n. bioavailability. DESIGN: Open‐label, randomized, five‐way cross‐over PK study. SETTING: Clinical trials facility (Croydon, UK). PARTICIPANTS: Thirty‐eight healthy volunteers (age 20–54 years; 11 female). INTERVENTION AND COMPARATOR: Three doses of i.n. (1 mg/0.1 ml, 2 mg/0.1 ml, 4 mg/0.2 ml) versus 0.4 mg i.m. (reference) and 0.4 mg intravenous (i.v.) naloxone. MEASUREMENTS: Regular blood samples were taken, with high‐frequency sampling during the first 15 minutes to capture early systemic exposure. PK parameters were determined from plasma naloxone concentrations. Exploratory analyses involved simulation of repeat administration. FINDINGS: Mean peak concentration (C(max)) values for 1 mg (1.51 ng/ml), 2 mg (2.87 ng/ml) and 4 mg (6.02 ng/ml) i.n. exceeded 0.4 mg i.m. (1.27 ng/ml) naloxone. All three i.n. doses rapidly achieved plasma levels > 50% of peak concentrations (T50%) by 10 minutes, peaking at 15–30 minutes (T(max)). For comparison, the i.m. reference reached T(max) at 10 minutes. Mean bioavailability was 47–51% for i.n. relative to i.m. naloxone. Simulation of repeat dosing (2 × 2 mg i.n. versus 5 × 0.4 mg i.m. doses) at 3‐minute intervals showed that comparable plasma naloxone concentrations would be anticipated. CONCLUSIONS: Concentrated 2 mg intranasal naloxone is well‐absorbed and provides early exposure comparable to 0.4 mg intramuscular naloxone, following the 0.4 mg intramuscular curve closely in the first 10 minutes post‐dosing and maintaining blood levels above twice the intramuscular reference for the next 2 hours.
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spelling pubmed-58369742018-03-12 Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study McDonald, Rebecca Lorch, Ulrike Woodward, Jo Bosse, Björn Dooner, Helen Mundin, Gill Smith, Kevin Strang, John Addiction Research Reports BACKGROUND AND AIMS: Take‐home naloxone can prevent death from heroin/opioid overdose, but pre‐provision is difficult because naloxone is usually given by injection. Non‐injectable alternatives, including naloxone nasal sprays, are currently being developed. To be effective, the intranasal (i.n.) spray dose must be adequate but not excessive, and early absorption must be comparable to intramuscular (i.m.) injection. We report on the pharmacokinetics (PK) of a specially produced concentrated novel nasal spray. The specific aims were to: (1) estimate PK profiles of i.n. naloxone, (2) compare early systemic exposure with i.n. versus i.m. naloxone and (3) estimate i.n. bioavailability. DESIGN: Open‐label, randomized, five‐way cross‐over PK study. SETTING: Clinical trials facility (Croydon, UK). PARTICIPANTS: Thirty‐eight healthy volunteers (age 20–54 years; 11 female). INTERVENTION AND COMPARATOR: Three doses of i.n. (1 mg/0.1 ml, 2 mg/0.1 ml, 4 mg/0.2 ml) versus 0.4 mg i.m. (reference) and 0.4 mg intravenous (i.v.) naloxone. MEASUREMENTS: Regular blood samples were taken, with high‐frequency sampling during the first 15 minutes to capture early systemic exposure. PK parameters were determined from plasma naloxone concentrations. Exploratory analyses involved simulation of repeat administration. FINDINGS: Mean peak concentration (C(max)) values for 1 mg (1.51 ng/ml), 2 mg (2.87 ng/ml) and 4 mg (6.02 ng/ml) i.n. exceeded 0.4 mg i.m. (1.27 ng/ml) naloxone. All three i.n. doses rapidly achieved plasma levels > 50% of peak concentrations (T50%) by 10 minutes, peaking at 15–30 minutes (T(max)). For comparison, the i.m. reference reached T(max) at 10 minutes. Mean bioavailability was 47–51% for i.n. relative to i.m. naloxone. Simulation of repeat dosing (2 × 2 mg i.n. versus 5 × 0.4 mg i.m. doses) at 3‐minute intervals showed that comparable plasma naloxone concentrations would be anticipated. CONCLUSIONS: Concentrated 2 mg intranasal naloxone is well‐absorbed and provides early exposure comparable to 0.4 mg intramuscular naloxone, following the 0.4 mg intramuscular curve closely in the first 10 minutes post‐dosing and maintaining blood levels above twice the intramuscular reference for the next 2 hours. John Wiley and Sons Inc. 2017-11-16 2018-03 /pmc/articles/PMC5836974/ /pubmed/29143400 http://dx.doi.org/10.1111/add.14033 Text en © 2017 The Authors. Addiction published by John Wiley & Sons Ltd on behalf of Society for the Study of Addiction. This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial (http://creativecommons.org/licenses/by-nc/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Research Reports
McDonald, Rebecca
Lorch, Ulrike
Woodward, Jo
Bosse, Björn
Dooner, Helen
Mundin, Gill
Smith, Kevin
Strang, John
Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title_full Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title_fullStr Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title_full_unstemmed Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title_short Pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: Phase I healthy volunteer study
title_sort pharmacokinetics of concentrated naloxone nasal spray for opioid overdose reversal: phase i healthy volunteer study
topic Research Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836974/
https://www.ncbi.nlm.nih.gov/pubmed/29143400
http://dx.doi.org/10.1111/add.14033
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