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愈创甘油醚和酮洛芬对热熔挤出聚环氧乙烷薄膜性能的影响。

The influence of guaifenesin and ketoprofen on the properties of hot-melt extruded polyethylene oxide films.

作者信息

Crowley Michael M, Fredersdorf Anke, Schroeder Britta, Kucera Shawn, Prodduturi Suneela, Repka Michael A, McGinity James W

机构信息

Division of Pharmaceutics, College of Pharmacy, The University of Texas at Austin, Austin, TX 78712, USA.

出版信息

Eur J Pharm Sci. 2004 Aug;22(5):409-18. doi: 10.1016/j.ejps.2004.04.005.

Abstract

Films containing polyethylene oxide (PEO) and a model drug, either guaifenesin (GFN) or ketoprofen (KTP), were prepared by hot-melt extrusion. The thermal properties of the hot-melt extruded films were investigated using differential scanning calorimetry (DSC). Scanning electron microscopy (SEM) was used to examine the surface morphology of the films, and wide angle X-ray diffraction (XRD) was used to investigate the crystalline properties of the polymer, drugs and physical mixtures as well as the solid state structure of the films. The stability of the polymer was studied using gel permeation chromatography. The mechanical properties, including percent elongation and tensile strength of the films, were determined on an Instron according to American Society for Testing Materials (ASTM) procedures. The Hansen solubility parameter was calculated using the Hoftyzer or van Krevelen method to estimate the likelihood of drug--polymer miscibility. Both GFN and KTP were stable during the extrusion process. Melting points corresponding to the crystalline drugs were not observed in the films. Crystallization of GFN on the surface of the film was observed at all concentrations studied, however KTP crystallization did not occur until reaching the 15% level. Guaifenesin and ketoprofen were found to decrease drive load, increase PEO stability and plasticize the polymer during extrusion. The Hansen solubility parameters predicted miscibility between PEO and KTP and poor miscibility between PEO and GFN. The predictions of the solubility parameters were in agreement with the XRD and SEM results. The percent elongation decreased with increasing GFN concentrations and significantly increased with increasing levels of KTP. Both GFN and KTP decreased the tensile strength of the extruded film.

摘要

通过热熔挤出法制备了含有聚环氧乙烷(PEO)和一种模型药物(愈创甘油醚(GFN)或酮洛芬(KTP))的薄膜。使用差示扫描量热法(DSC)研究了热熔挤出薄膜的热性能。扫描电子显微镜(SEM)用于检查薄膜的表面形态,广角X射线衍射(XRD)用于研究聚合物、药物和物理混合物的结晶性能以及薄膜的固态结构。使用凝胶渗透色谱法研究了聚合物的稳定性。根据美国材料与试验协会(ASTM)程序,在英斯特朗万能材料试验机上测定了薄膜的机械性能,包括伸长率和拉伸强度。使用霍夫蒂泽尔或范克雷维伦方法计算汉森溶解度参数,以估计药物与聚合物混溶的可能性。在挤出过程中,GFN和KTP均保持稳定。在薄膜中未观察到与结晶药物相对应的熔点。在所研究的所有浓度下,均观察到GFN在薄膜表面结晶,然而,直到达到15%的水平,KTP才发生结晶。发现愈创甘油醚和酮洛芬在挤出过程中会降低驱动负荷、提高PEO稳定性并使聚合物增塑。汉森溶解度参数预测PEO与KTP之间可混溶,而PEO与GFN之间混溶性较差。溶解度参数的预测结果与XRD和SEM结果一致。伸长率随GFN浓度的增加而降低,随KTP含量的增加而显著增加。GFN和KTP均降低了挤出薄膜的拉伸强度。

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