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Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release

Clay–polymer nanocomposites have exhibited a great potential as carriers for controlled release drug delivery. This study aims to prepare exfoliated montmorillonite–Eudragit RS nanocomposites using reactive melt extrusion and investigate the influence of claying loading, clay types (sodium montmoril...

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Autores principales: Liu, Xu, Lu, Xingyu, Su, Yongchao, Kun, Eucharist, Zhang, Feng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7022276/
https://www.ncbi.nlm.nih.gov/pubmed/31936176
http://dx.doi.org/10.3390/pharmaceutics12010051
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author Liu, Xu
Lu, Xingyu
Su, Yongchao
Kun, Eucharist
Zhang, Feng
author_facet Liu, Xu
Lu, Xingyu
Su, Yongchao
Kun, Eucharist
Zhang, Feng
author_sort Liu, Xu
collection PubMed
description Clay–polymer nanocomposites have exhibited a great potential as carriers for controlled release drug delivery. This study aims to prepare exfoliated montmorillonite–Eudragit RS nanocomposites using reactive melt extrusion and investigate the influence of claying loading, clay types (sodium montmorillonite (Cloisite Na) vs. organomodified montmorillonite (Cloisite 20)) on clay–polymer interactions and drug release properties. The clays were used as the filler material at various levels in Eudragit RS and theophylline was used as the active pharmaceutical ingredient. The resulting structure of the nanocomposites was characterized using TEM (transmission electron microscopy) and XRPD (X-ray powder diffraction). The hygroscopicity of the nanocomposites was investigated using DVS (dynamic vapor sorption). The effect of the interfacial interaction between the polymer and clay sheet, the clay loading as well as the clay type on the drug release behavior were further studied by dissolution testing. TEM and XRPD data show that when the clay content is increased from 5% to 15% by weight, the nanocomposite’s structure switches from a fully exfoliated state to intercalated structures or partial exfoliation with stacked clay layers. FT-IR (fourier transform infrared spectroscopy) and ssNMR (solid-state NMR) results suggest that Cloisite Na and Cloisite 20 layers exhibit different interaction strengths with polymer networks by creating compacted complex structures. The addition of nanoclay in the formulation could robustly adjust drug release profiles, and the clay concentration and type are important factors that affect the crossing-linking density of the nanocomposites by adjusting the drug release properties. This study indicates that the clay–Eudragit RS nanocomposites provide an improved oral controlled drug delivery system that minimizes the drug dosing frequency, potentially leading to improved patient compliance.
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spelling pubmed-70222762020-03-09 Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release Liu, Xu Lu, Xingyu Su, Yongchao Kun, Eucharist Zhang, Feng Pharmaceutics Article Clay–polymer nanocomposites have exhibited a great potential as carriers for controlled release drug delivery. This study aims to prepare exfoliated montmorillonite–Eudragit RS nanocomposites using reactive melt extrusion and investigate the influence of claying loading, clay types (sodium montmorillonite (Cloisite Na) vs. organomodified montmorillonite (Cloisite 20)) on clay–polymer interactions and drug release properties. The clays were used as the filler material at various levels in Eudragit RS and theophylline was used as the active pharmaceutical ingredient. The resulting structure of the nanocomposites was characterized using TEM (transmission electron microscopy) and XRPD (X-ray powder diffraction). The hygroscopicity of the nanocomposites was investigated using DVS (dynamic vapor sorption). The effect of the interfacial interaction between the polymer and clay sheet, the clay loading as well as the clay type on the drug release behavior were further studied by dissolution testing. TEM and XRPD data show that when the clay content is increased from 5% to 15% by weight, the nanocomposite’s structure switches from a fully exfoliated state to intercalated structures or partial exfoliation with stacked clay layers. FT-IR (fourier transform infrared spectroscopy) and ssNMR (solid-state NMR) results suggest that Cloisite Na and Cloisite 20 layers exhibit different interaction strengths with polymer networks by creating compacted complex structures. The addition of nanoclay in the formulation could robustly adjust drug release profiles, and the clay concentration and type are important factors that affect the crossing-linking density of the nanocomposites by adjusting the drug release properties. This study indicates that the clay–Eudragit RS nanocomposites provide an improved oral controlled drug delivery system that minimizes the drug dosing frequency, potentially leading to improved patient compliance. MDPI 2020-01-07 /pmc/articles/PMC7022276/ /pubmed/31936176 http://dx.doi.org/10.3390/pharmaceutics12010051 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Liu, Xu
Lu, Xingyu
Su, Yongchao
Kun, Eucharist
Zhang, Feng
Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title_full Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title_fullStr Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title_full_unstemmed Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title_short Clay-Polymer Nanocomposites Prepared by Reactive Melt Extrusion for Sustained Drug Release
title_sort clay-polymer nanocomposites prepared by reactive melt extrusion for sustained drug release
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7022276/
https://www.ncbi.nlm.nih.gov/pubmed/31936176
http://dx.doi.org/10.3390/pharmaceutics12010051
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