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Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces

[Image: see text] The preparation of thin composite layers has promising advantages in a variety of applications like transdermal, buccal, or sublingual patches. Within this model study the impact of the matrix material on the film forming properties of ibuprofen–matrix composite films is investigat...

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Autores principales: Kellner, Thomas, Ehmann, Heike M. A., Schrank, Simone, Kunert, Birgit, Zimmer, Andreas, Roblegg, Eva, Werzer, Oliver
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2014
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4223873/
https://www.ncbi.nlm.nih.gov/pubmed/25275801
http://dx.doi.org/10.1021/mp500264e
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author Kellner, Thomas
Ehmann, Heike M. A.
Schrank, Simone
Kunert, Birgit
Zimmer, Andreas
Roblegg, Eva
Werzer, Oliver
author_facet Kellner, Thomas
Ehmann, Heike M. A.
Schrank, Simone
Kunert, Birgit
Zimmer, Andreas
Roblegg, Eva
Werzer, Oliver
author_sort Kellner, Thomas
collection PubMed
description [Image: see text] The preparation of thin composite layers has promising advantages in a variety of applications like transdermal, buccal, or sublingual patches. Within this model study the impact of the matrix material on the film forming properties of ibuprofen–matrix composite films is investigated. As matrix materials polystyrene, methyl cellulose, or hydroxyl-ethyl cellulose were used. The film properties were either varied by the preparation route, i.e., spin coating or drop casting, or via changes in the relative ratio of the ibuprofen and the matrix material. The resulting films were investigated via X-ray diffraction and atomic force microscope experiments. The results show that preferred (100) textures can be induced via spin coating with respect to the glass surface, while the drop casting results in a powder-like behavior. The morphologies of the films are strongly impacted by the ibuprofen amount rather than the preparation method. A comparison of the various matrix materials in terms of their impact on the dissolution properties show a two times faster zero order release from methyl cellulose matrix compared to a polystyrene matrix. The slowest rate was observed within the hydroxyl ethyl cellulose as the active pharmaceutical ingredients (APIs) release is limited by diffusion through a swollen matrix. The investigation reveals that the ibuprofen crystallization and film formation is only little effected by the selected matrix material than that compared to the dissolution. A similar experimental approach using other matrix materials may therefore allow to find an optimized composite layer useful for a defined application.
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spelling pubmed-42238732014-11-09 Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces Kellner, Thomas Ehmann, Heike M. A. Schrank, Simone Kunert, Birgit Zimmer, Andreas Roblegg, Eva Werzer, Oliver Mol Pharm [Image: see text] The preparation of thin composite layers has promising advantages in a variety of applications like transdermal, buccal, or sublingual patches. Within this model study the impact of the matrix material on the film forming properties of ibuprofen–matrix composite films is investigated. As matrix materials polystyrene, methyl cellulose, or hydroxyl-ethyl cellulose were used. The film properties were either varied by the preparation route, i.e., spin coating or drop casting, or via changes in the relative ratio of the ibuprofen and the matrix material. The resulting films were investigated via X-ray diffraction and atomic force microscope experiments. The results show that preferred (100) textures can be induced via spin coating with respect to the glass surface, while the drop casting results in a powder-like behavior. The morphologies of the films are strongly impacted by the ibuprofen amount rather than the preparation method. A comparison of the various matrix materials in terms of their impact on the dissolution properties show a two times faster zero order release from methyl cellulose matrix compared to a polystyrene matrix. The slowest rate was observed within the hydroxyl ethyl cellulose as the active pharmaceutical ingredients (APIs) release is limited by diffusion through a swollen matrix. The investigation reveals that the ibuprofen crystallization and film formation is only little effected by the selected matrix material than that compared to the dissolution. A similar experimental approach using other matrix materials may therefore allow to find an optimized composite layer useful for a defined application. American Chemical Society 2014-10-02 2014-11-03 /pmc/articles/PMC4223873/ /pubmed/25275801 http://dx.doi.org/10.1021/mp500264e Text en Copyright © 2014 American Chemical Society This is an open access article published under a Creative Commons Attribution (CC-BY) License (http://pubs.acs.org/page/policy/authorchoice_ccby_termsofuse.html) , which permits unrestricted use, distribution and reproduction in any medium, provided the author and source are cited.
spellingShingle Kellner, Thomas
Ehmann, Heike M. A.
Schrank, Simone
Kunert, Birgit
Zimmer, Andreas
Roblegg, Eva
Werzer, Oliver
Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title_full Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title_fullStr Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title_full_unstemmed Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title_short Crystallographic Textures and Morphologies of Solution Cast Ibuprofen Composite Films at Solid Surfaces
title_sort crystallographic textures and morphologies of solution cast ibuprofen composite films at solid surfaces
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4223873/
https://www.ncbi.nlm.nih.gov/pubmed/25275801
http://dx.doi.org/10.1021/mp500264e
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