雷米普利三层基质缓释片的制备及实验设计评价

K. Ashwin, T. R. Reddy, P. Nirmala
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引用次数: 0

摘要

本研究旨在设计、制备和评价拉米普利三层基质缓释片的缓释效果。采用直接压缩法,采用33响应面法对不同浓度的HPMC K4M、HPMC K15M和黄原胶(低、中、高浓度)聚合物制备活性层(中间层)的27个配方(RF1-RF27)。根据该制剂的理化性质和药物释放特性,选择一种制剂,采用直接压缩法将不同比例的聚合物配制成缓释片,并对其进行评价。对最佳配方进行了FTIR表征。在27个活性层剂型中,选择RF23为最优剂型,最大释药率为98.11%,通过不同比例的聚合物配制成三层基质缓释片(ARF23-HRF23)。各批次(ARF23-HRF23)溶肿指数范围为82.34 ~ 97.46%,药物含量范围为95.49 ~ 99.11%,24小时持续释放药物范围为84.98 ~ 98.26%,GRF23均为最高。释放顺序动力学数据表明,GRF23的零级释放最高(R2) = 0.983,优于市售一阶产品,R2值为0.962。此外,公式(GRF23)最适合Korsmeyer-Peppas图,即0.957表示非菲克(异常)输移耦合扩散和侵蚀。FT-IR数据保证了药物和辅料的相容性。发现GRF23在加速条件下稳定180天。
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Preparation and Evaluation of Extended Release Trilayered Matrix Tablets of Ramipril Using Design of Experiment
The current work is aimed to design, prepare, and evaluate the trilayer matrix tablets incorporated with ramipril for extended drug release. Twenty-seven formulations (RF1-RF27) for active layer (middle layer) were prepared by direct compression method using 33 Response surface method of polymers of different HPMC K4M, HPMC K15M and xanthan gum (low, middle, and high concentrations) by using Design of experiment software. Based on physico-chemical properties and drug release one formulation was chosen and formulated into extended release trilayered matrix tablets were by varying proportions of polymers by direct compression method and they were evaluated. The best optimized formulation was characterized for FTIR studies. Out of 27 active layer formulations, RF23 was chosen as best based with maximum drug release of 98.11% and was formulated into extended release trilayered matrix tablets (ARF23-HRF23) by varying proportions of polymers. The range of swelling index for all batches (ARF23-HRF23) was 82.34 to 97.46%, similarly the range of drug content was 95.49 to 99.11% and drug released in 24 hours sustainably over an extended period was 84.98 to 98.26% with all highest values exhibited by GRF23. The release order kinetics data indicate the zero-order release with highest (R2) = 0.983 for GRF23 better when compared to marketed product which followed first order showed R2 value 0.962. Further the formulation (GRF23) showed best fit to Korsmeyer-Peppas plots i.e., 0.957 indicating non Fickian (anomalous) transport coupled diffusion and erosion. The FT-IR data assure the compatibilityof drug and excipients. GRF23 was found to be stable for 180 days at accelerated conditions.
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