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Indomethacin-Kollidon VA64 Extrudates: A Mechanistic Study of pH-Dependent Controlled Release

Wren, Stephen A. C.; Aylott, Jonathan W.; Tres, Francesco; Treacher, Kevin; Booth, Jonathan; Hughes, Leslie P.; Wren, Stephen A.C.; Aylott, Jonathan; Burley, Jonathan C.

Authors

Stephen A. C. Wren

Jonathan W. Aylott

Francesco Tres

Kevin Treacher

Jonathan Booth

Leslie P. Hughes

Stephen A.C. Wren



Abstract

© 2016 American Chemical Society. Because of its weakly acidic nature (pKa of 4.5), indomethacin presents an aqueous solubility that significantly increases when changing from acidic to neutral/alkaline pH (1.5 μg/mL at pH 1.2 and 105.2 μg/mL at pH 7.4). We have therefore investigated the impact of the dissolution medium pH on the dissolution performance of indomethacin:Kollidon VA64 extrudates. The impact of the drug loading on the dissolution properties of these systems was also examined (5%, 15%, 30%, 50%, 70%, and 90% drug loading). Time-resolved Raman spectroscopy along with in-line UV-vis spectrophotometry was employed to directly relate changes in dissolution behavior to physicochemical changes that occur to the extrudate during the test. The dissolution tests were performed in pH 2 HCl (to mimic the stomach conditions), and this was then switched during the experiment to pH 6.8 phosphate buffer (to simulate the poststomach conditions). The rotating disc dissolution rate test was also used to simultaneously measure the dissolution rate of both the drug and the polymer. We found that in pH 2 HCl buffer, for the 15% or higher drug-loaded extrudates, Kollidon VA64 preferentially dissolves from the exterior of the compact leaving an amorphous drug-rich hydrophobic shell, which, similarly to an enteric coating, inhibits the drug release. The in situ formation of an enteric coating has been previously hypothesized, and this has been the first time that is directly observed in a pH-variable dissolution test. The dissolution medium switch to pH 6.8 phosphate buffer, due to the large increase of the aqueous solubility of indomethacin at this pH, leads to rapid dissolution of the material forming the coating and therefore total drug release. In contrast, the 5% extrudate is fully hydrated and quickly dissolves at low pH pointing to a dissolution performance dependent on highly water-soluble Kollidon VA64.

Journal Article Type Article
Acceptance Date Feb 4, 2016
Online Publication Date Feb 18, 2016
Publication Date Mar 7, 2016
Deposit Date May 10, 2018
Journal Molecular Pharmaceutics
Print ISSN 1543-8384
Electronic ISSN 1543-8392
Publisher American Chemical Society
Peer Reviewed Peer Reviewed
Volume 13
Issue 3
Pages 1166-1175
DOI https://doi.org/10.1021/acs.molpharmaceut.5b00979
Public URL https://nottingham-repository.worktribe.com/output/1109527
Publisher URL https://pubs.acs.org/doi/10.1021/acs.molpharmaceut.5b00979#
PMID 00037175