乙酰氯芬酸定时压包脉冲治疗系统:影响药物释放和延迟时间的因素优化

Sumit T. Patil, S. Pund, A. Joshi, C. Shishoo, Aliasgar F. Shahiwala
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引用次数: 17

摘要

DOI: 10.2147 / CPT。背景:本研究的目的是开发和评估一种压包搏动给药系统,用于治疗类风湿性关节炎患者的清晨僵硬和疼痛症状缓解。方法:制定相关新闻的涂层可破裂的外套在迅速d isintegrating aceclofenac的核心的平板电脑。采用三因素、二水平、全因子设计,考察了包衣成分中甘油三酯的用量、氯化钠的用量和包衣水平对反应的影响,即释放滞后时间和450 min内乙酰氯芬酸的释放量。结果:甘油酯和涂层水平对滞后时间有显著影响,而氯化钠作为通道剂有助于涂层的破裂。涂层破裂后,由于Ac-Di-Sol的存在,芯片显示出乙酰氯芬酸的快速释放。通过Lenth方法和贝叶斯系数分析对效果进行图形分析,可以识别对选定响应起作用的变量。优化后的配方由20% w/w的甘油酸酯和2.2% w/w的氯化钠组成,包衣量为650 mg,延迟时间为358.23分钟,模拟类风湿关节炎的波动症状,随后迅速释放乙酰氯芬酸。
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Chronomodulated press-coated pulsatile therapeutic system for aceclofenac: optimization of factors influencing drug release and lag time
DOI: 10.2147/CPT.S16504 Background: The objective of this study was to develop and evaluate a press-coated pulsatile drug delivery system intended for treatment of early morning stiffness and symptomatic relief from pain in patients with rheumatoid arthritis. Methods: The formulation involved press coating of a rupturable coat around a rapidly d isintegrating core tablet of aceclofenac. A three-factor, two-level, full factorial design was used to i nvestigate the influence of amount of glyceryl behenate, amount of sodium chloride in the coating c omposition, and the coating level on the responses, ie, lag time to release and amount of aceclofenac released in 450 minutes. Results: Glyceryl behenate and the coating level had a significant influence on lag time, while sodium chloride helped in the rupture of the coat by acting as a channeling agent. After the coat was ruptured, the core tablet showed a rapid release of aceclofenac due to the presence of Ac-Di-Sol. Graphical analysis of effects by Lenth’s method and Bayesian analysis of coefficients enabled identification of variables active on the selected responses. The optimized formulation comprised 20% w/w glyceryl behenate and 2.2% w/w sodium chloride with a 650 mg coating level, and showed a desired lag time of 358.23 minutes, which mimics the fluctuating symptoms of rheumatoid arthritis, followed by rapid release of aceclofenac.
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