Improvement of dissolution and tabletability of carbamazepine solid dispersions with high drug loading prepared by hot-melt extrusion.

Zilin Feng, Mengting Li, Wenxi Wang
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引用次数: 9

Abstract

Solid dispersions (SDs) have made great progress in the improvement of dissolution for poorly soluble drugs, however the low drug loading still limits their wide application. In the present paper, high carbamazepine (CBZ) loaded SDs with excellent dissolution and tabletability were prepared and characterized. The CBZ SDs were prepared with Eudragit EPO as carrier by hot-melt extrusion (HME) in the drug: carrier ratio of 4:1. Powder X-ray diffraction, differential scanning calorimetry, fourier transform infrared spectroscopy and powder dissolution was carried out to characterize the SDs. The results showed that the crystalline form the polymorph of CBZ in SDs was transformed into form I from form III after extruded at 140 °C. Wettability and microstructure of CBZ SDs were improved by the HME process, which promoted the dissolution significantly. More than 85 % drug dissolved within 5 min from CBZ SDs with even only 20 % Eudragit EPO as carrier. CBZ SDs tablets were prepared by direct tableting with a universal material testing machine at various compaction pressures. Compactibility and tabletability were enhanced significantly by the HME process. All of these results showed the CBZ SDs prepared by HME with 80 % CBZ and 20 % Eudragit EPO could improve the dissolution and tabletability significantly.
热熔挤压法制备卡马西平高载药量固体分散体的溶出性和给药性的改进。
固体分散体(SDs)在改善难溶性药物的溶出度方面取得了很大的进展,但由于载药量低,限制了其广泛应用。本文制备了高卡马西平负载SDs,并对其进行了表征。以尤德拉吉EPO为载体,在药物载体比为4:1的条件下,采用热熔挤压法制备CBZ SDs。采用粉末x射线衍射、差示扫描量热法、傅里叶变换红外光谱和粉末溶出度等方法对SDs进行表征。结果表明:在140℃挤压后,SDs中CBZ的晶型由III型转变为I型;HME工艺改善了CBZ SDs的润湿性和微观结构,显著促进了其溶解。85%以上的药物在5分钟内从CBZ SDs中溶解,甚至只有20%的Eudragit EPO作为载体。采用通用材料试验机在不同压实压力下直接压片法制备CBZ SDs片。HME工艺显著提高了产品的亲和性和可制表性。结果表明,以80%的CBZ和20%的Eudragit EPO为原料,HME法制备的CBZ SDs可显著提高其溶出度和溶出性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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