Preparation and Evaluation of Sustained-Release Matrix Tablets Based on Metoprolol and an Acrylic Carrier Using Injection Moulding

被引:0
|
作者
T. Quinten
G. P. Andrews
T. De Beer
L. Saerens
W. Bouquet
D. S. Jones
P. Hornsby
J. P. Remon
C. Vervaet
机构
[1] Ghent University,Laboratory of Pharmaceutical Technology
[2] Queen’s University Belfast,School of Pharmacy
[3] Ghent University,Laboratory of Pharmaceutical Process Analytical Technology
[4] Queen’s University Belfast,School of Mechanical and Aerospace Engineering
来源
AAPS PharmSciTech | 2012年 / 13卷
关键词
acrylates; controlled release; drug polymer interaction; drug release; injection moulding; matrix; metoprolol; physicochemical properties; solid state; sustained release; tablet;
D O I
暂无
中图分类号
学科分类号
摘要
Sustained-release matrix tablets based on Eudragit RL and RS were manufactured by injection moulding. The influence of process temperature; matrix composition; drug load, plasticizer level; and salt form of metoprolol: tartrate (MPT), fumarate (MPF) and succinate (MPS) on ease of processing and drug release were evaluated. Formulations composed of 70/30% Eudragit RL/MPT showed the fastest drug release, substituting part of Eudragit RL by RS resulted in slower drug release, all following first-order release kinetics. Drug load only affected drug release of matrices composed of Eudragit RS: a higher MPT concentration yielded faster release rates. Adding triethyl citrate enhanced the processability, but was detrimental to long-term stability. The process temperature and plasticizer level had no effect on drug release, whereas metoprolol salt form significantly influenced release properties. The moulded tablets had a low porosity and a smooth surface morphology. A plasticizing effect of MPT, MPS and MPF on Eudragit RS and Eudragit RL was observed via DSC and DMA. Solubility parameter assessment, thermal analysis and X-ray diffraction demonstrated the formation of a solid solution immediately after production, in which H-bonds were formed between metoprolol and Eudragit as evidenced by near-infrared spectroscopy. However, high drug loadings of MPS and MPF showed a tendency to recrystallise during storage. The in vivo performance of injection-moulded tablets was strongly dependent upon drug loading.
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页码:1197 / 1211
页数:14
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