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基于与聚乙二醇6000和表面活性剂的三元固体分散体的格列本脲速溶片。

Fast-dissolving tablets of glyburide based on ternary solid dispersions with PEG 6000 and surfactants.

作者信息

Cirri Marzia, Maestrelli Francesca, Corti Giovanna, Mura Paola, Valleri Maurizio

机构信息

Department of Pharmaceutical Sciences, University of Florence, Firenze, Italy.

出版信息

Drug Deliv. 2007 Apr;14(4):247-55. doi: 10.1080/10717540601067802.

Abstract

Marketed glyburide tablets present unsatisfying dissolution profiles that give rise to variable bioavailability. With the purpose of developing a fast-dissolving tablet formulation able to assure a complete drug dissolution, we investigated the effect of the addition to a reference tablet formulation of different types (anionic and nonionic) and amounts of hydrophilic surfactants, as well as the use of a new technique, based on ternary solid dispersions of the drug with an hydrophilic carrier (polyethylene glycol [PEG] 6000) and a surfactant. Tablets were prepared by direct compression or previous wet granulation of suitable formulations containing the drug with each surfactant or drug:PEG:surfactant ternary dispersions at different PEG:surfactant w/w ratios. The presence of surfactants significantly increased (p<0.01) the drug dissolution rate, but complete drug dissolution was never achieved. On the contrary, in all cases tablets containing ternary solid dispersions achieved 100% dissolved drug within 60 min. The best product was the 10:80:10 w/w ternary dispersion with PEG 6000 and sodium laurylsulphate, showing a dissolution efficiency 5.5-fold greater than the reference tablet formulation and 100% drug dissolution after only 20 min.

摘要

市售的格列本脲片呈现出不尽人意的溶出曲线,导致生物利用度参差不齐。为了开发一种能够确保药物完全溶解的速溶片制剂,我们研究了向参比片制剂中添加不同类型(阴离子型和非离子型)及不同用量的亲水性表面活性剂的效果,以及基于药物与亲水性载体(聚乙二醇 [PEG] 6000)和表面活性剂的三元固体分散体的新技术的应用。通过直接压片或对含有药物与每种表面活性剂或药物:PEG:表面活性剂三元分散体(不同PEG:表面活性剂重量比)的合适制剂进行先前的湿法制粒来制备片剂。表面活性剂的存在显著提高了(p<0.01)药物溶出速率,但从未实现药物完全溶解。相反,在所有情况下,含有三元固体分散体的片剂在60分钟内实现了100%药物溶解。最佳产品是含PEG 6000和十二烷基硫酸钠的10:80:10重量比的三元分散体,其溶出效率比参比片制剂高5.5倍,仅20分钟后药物溶解率就达到100%。

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