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Predictability of drug release from water-insoluble polymeric matrix tablets

机译:水不溶性聚合物基质片剂中药物释放的可预测性

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The purpose of this study was to extend the predictability of an established solution of Fick's second law of diffusion with formulation-relevant parameters and including percolation theory. Kollidon SR (polyvinyl acetate/polyvinylpyrrolidone, 80/20 w/w) matrix tablets with various porosities (10-30% v/v) containing model drugs with different solubilities (Cs = 10-170 mg/ml) and in different amounts (A = 10-90% w/w) were prepared by direct compression and characterized by drug release and mass loss studies. Drug release was fitted to Fick's second law to obtain the apparent diffusion coefficient. Its changes were correlated with the total porosity of the matrix and the solubility of the drug. The apparent diffusion coefficient was best described by a cumulative normal distribution over the range of total porosities. The mean of the distribution coincided with the polymer percolation threshold, and the minimum and maximum of the distribution were represented by the diffusion coefficient in pore-free polymer and in aqueous medium, respectively. The derived model was verified, and the applicability further extended to a drug solubility range of 10-1000 mg/ml. The developed mathematical model accurately describes and predicts drug release from Kollidon SR matrix tablets. It can efficiently reduce experimental trials during formulation development.
机译:这项研究的目的是通过公式相关参数并包括渗流理论来扩展菲克第二扩散定律的既定解决方案的可预测性。具有不同孔隙率(10-30%v / v)的Kollidon SR(聚乙酸乙烯酯/聚乙烯吡咯烷酮,80/20 w / w)基质片剂,包含具有不同溶解度(Cs = 10-170 mg / ml)和不同量的模型药物( A = 10-90%w / w)通过直接压缩制备,并通过药物释放和质量损失研究进行表征。使药物释放符合菲克第二定律以获得表观扩散系数。其变化与基质的总孔隙率和药物的溶解度相关。表观扩散系数最好用总孔隙率范围内的累积正态分布来描述。分布的平均值与聚合物的渗滤阈值一致,并且分布的最小值和最大值分别由无孔聚合物和水性介质中的扩散系数表示。验证了衍生的模型,并且适用性进一步扩展到10-1000 mg / ml的药物溶解度范围。建立的数学模型可准确描述和预测Kollidon SR基质片剂的药物释放。它可以有效地减少配方开发过程中的实验。

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