Population Pharmacokinetic Analysis Supports Initiation Treatment and Bridging from Sublingual Buprenorphine to Subcutaneous Administration of a Buprenorphine Depot (CAM2038) in the Treatment of Opioid Use Disorder.

Marcus Björnsson Chayan Acharya Kerstin Strandgården Fredrik Tiberg

Clin Pharmacokinet

Camurus AB, Lund, Sweden.

Published: October 2023

Subcutaneous (SC) extended-release buprenorphine (BPN), like CAM2038, offers more stable plasma levels and improved treatment outcomes for opioid use disorder (OUD) compared to daily sublingual (SL) BPN.
A population pharmacokinetic (PK) model was created using data from trials involving 252 participants, showing that BPN is best described by a three-compartment model and can be absorbed through dual pathways.
The model supports the use of personalized CAM2038 dosing for OUD treatment, including during the initiation, switch from SL BPN, and tapering phases.

Background And Objective: In treating opioid use disorder (OUD), subcutaneous (SC) extended-release buprenorphine (BPN) depots, e.g., CAM2038, have been shown to provide smaller and less frequent fluctuations in BPN plasma concentrations and pharmacodynamic responses, improve outcomes, reduce treatment burden, and lower risks of misuse and diversion compared to daily sublingual (SL) BPN. This analysis characterized the pharmacokinetics (PK) of BPN following intravenous and SL administration, and administration of SC CAM2038 weekly and monthly.

Methods: Pharmacokinetic data from two Phase 1 and two Phase 2 trials in healthy participants and participants with OUD, respectively, were used to develop a population PK model using non-linear mixed effects modelling. The analysis included data from 252 participants and 10,658 BPN observations.

Results: The disposition of BPN was best described by a three-compartment model with first-order elimination, and absorption of SL BPN and SC CAM2038 weekly and monthly by dual parallel absorption pathways. Model diagnostics indicated good predictive performance of BPN concentrations. Buprenorphine plasma concentration-time profiles were simulated for treatment initiation, switching from SL BPN to CAM2038 weekly and monthly, and tapering after interrupting treatment with CAM2038. Simulations predicted CAM2038 weekly and monthly doses that provided BPN plasma maximum concentration (C) and trough concentration (C) values at steady state within those observed following SL BPN administration.

Conclusions: This population PK model supports the use of CAM2038 doses as individualized treatment for OUD across different treatment stages, including initiation, switching from SL BPN according to established dose conversion schedules, and tapering.

Trial Registrations: ISRCTN41550730 (05/19/2014), ISRCTN24987553 (07/29/2014), NCT02611752 (11/23/2015), NCT02710526 (03/16/2016).

Download full-text PDF	Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10520114	PMC
http://dx.doi.org/10.1007/s40262-023-01288-6	DOI Listing

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