Development of a 3D-Printed Dosing Platform to Aid in Zolpidem Withdrawal Therapy

Silke Henry; Lien De Vadder; Milan Decorte; Susanna Francia; Magali Van Steenkiste; Jan Saevels; Valérie Vanhoorne; Chris Vervaet

doi:10.3390/pharmaceutics13101684

Development of a 3D-Printed Dosing Platform to Aid in Zolpidem Withdrawal Therapy

Pharmaceutics. 2021 Oct 14;13(10):1684. doi: 10.3390/pharmaceutics13101684.

Authors

Silke Henry¹, Lien De Vadder¹, Milan Decorte¹, Susanna Francia², Magali Van Steenkiste³, Jan Saevels³, Valérie Vanhoorne¹, Chris Vervaet¹

Affiliations

¹ Laboratory of Pharmaceutical Technology, Ghent University, 9000 Ghent, Belgium.
² Laboratory of Pharmaceutical Technology, Università Di Pavia, 27100 Pavia, Italy.
³ Algemene Pharmaceutische Bond, 1000 Brussels, Belgium.

Abstract

The long-term use of benzodiazepine receptor agonists (BZRAs) is associated with multiple side effects, such as increased sedation, hangover or an elevated risk of dependency and abuse. Unfortunately, the long-term use of BZRAs is reaching worrying intake rates, and therefore, the need for action is high. It was demonstrated already that the overall willingness of patients for deprescription increased when a slow dose reduction scheme with the possibility for dose increase, if needed, is employed. The current study aims to develop a flexible dosing platform of zolpidem hemitartrate (ZHT) to facilitate such withdrawal therapy. As this is the first report on the extrusion and 3D printing of ZHT, its thermal behaviour and sensitivity towards photolytic degradation was characterised. It was shown that ZHT possesses multiple polymorphs and was especially prone to oxidative photolysis. Next, a variety of immediate release polymers (Eudragit EPO, Kollidon VA64, Kollidon 12PF and Soluplus) were blended and extruded with Polyox WSR N10 to investigate their feedability and printability by mechanical and rheological analysis. The addition of PEO was shown to enable printing of these brittle pharmaceutical polymers, although the processing temperature was deemed critical to avoid surface defects on the resulting filaments. An EPO(70)PEO(30) system was selected based on its suitable mechanical properties and low hygroscopicity favoring ZHT stability. The matrix was blended with 1% or 10% API. The effect of certain printing parameters (caplet size, nozzle diameter, % overlap) on dissolution behaviour and caplet weight/dimensions/quality was assessed. A flexible dosing platform capable of delivering <1 mg and up to 10 mg of ZHT was created. Either caplet modification (incorporation of channels) or disintegrant addition (Primojel, Explotab, Ac-Di-Sol, Primellose and Polyplasdone-XL) failed to achieve an immediate release profile. This study provides the first report of a 3D-printed flexible dosing platform containing ZHT to aid in withdrawal therapy.

Keywords: 3D printing; extrusion; fused deposition modeling; personalised medicine; zolpidem.

Grants and funding

HBC.2020.2203/Flanders Innovation and Entrepreneurship