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骨架片中药物渗透阈值与粒径的关系。

Relationship between drug percolation threshold and particle size in matrix tablets.

作者信息

Caraballo I, Millan M, Rabasco A M

机构信息

Department of Pharmacy and Pharmaceutical Technology, Faculty of Pharmacy, University of Seville, Spain.

出版信息

Pharm Res. 1996 Mar;13(3):387-90. doi: 10.1023/a:1016088424993.

Abstract

PURPOSE

Since a previous qualitative study carried out by us showed the existence of an important influence of the particle size on the percolation thresholds and taking into account that the existing theoretical models can only provide qualitative explanation to this influence, the purpose of this work is to carry out the first quantitative study of the influence of the particle size over the drug percolation thresholds.

METHODS

Matrix tablets have been elaborated using potassium chloride as drug model and Eudragit RS-PM as matrix forming material. Five different KCl particle size fractions have been employed whereas the Eudragit RS-PM particle size was kept constant. In-vitro release assays were carried out for all the elaborated lots. The drug percolation thresholds were estimated following the method proposed by Bonny and Leuenberger.

RESULTS

A linear relationship has been found between the drug particle size and the corresponding drug percolation threshold.

CONCLUSIONS

This finding confirms the results previously obtained in our qualitative study and has important repercussions in the design of pharmaceutical solid dosage forms. If this linear behaviour is general, the percolation threshold can soon become a useful preformulation parameter.

摘要

目的

由于我们之前进行的一项定性研究表明粒径对渗滤阈值存在重要影响,并且考虑到现有的理论模型只能对这种影响提供定性解释,因此本研究的目的是首次对粒径对药物渗滤阈值的影响进行定量研究。

方法

以氯化钾为药物模型,以丙烯酸树脂RS-PM为基质形成材料制备了基质片剂。采用了五种不同的氯化钾粒径级分,而丙烯酸树脂RS-PM的粒径保持恒定。对所有制备的批次进行了体外释放试验。按照Bonny和Leuenberger提出的方法估计药物渗滤阈值。

结果

发现药物粒径与相应的药物渗滤阈值之间存在线性关系。

结论

这一发现证实了我们之前在定性研究中获得的结果,并且对药物固体剂型的设计具有重要影响。如果这种线性行为具有普遍性,渗滤阈值很快就会成为一个有用的处方前参数。

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