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An optimized probucol microencapsulated formulation integrating a secondary bile acid (deoxycholic acid) as a permeation enhancer

机译:优化的普罗布考微囊化配方,整合了仲胆汁酸(脱氧胆酸)作为渗透促进剂

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Abstract: The authors have previously designed, developed, and characterized a novel microencapsulated formulation as a platform for the targeted delivery of therapeutics in an animal model of type 2 diabetes, using the drug probucol (PB). The aim of this study was to optimize PB microcapsules by incorporating the bile acid deoxycholic acid (DCA), which has good permeation-enhancing properties, and to examine its effect on microcapsules’ morphology, rheology, structural and surface characteristics, and excipients’ chemical and thermal compatibilities. Microencapsulation was carried out using a BüCHI-based microencapsulating system established in the authors’ laboratory. Using the polymer sodium alginate (SA), two microencapsulated formulations were prepared: PB-SA (control) and PB-DCA-SA (test) at a constant ratio (1:30 and 1:3:30, respectively). Complete characterization of the microcapsules was carried out. The incorporation of DCA resulted in better structural and surface characteristics, uniform morphology, and stable chemical and thermal profiles, while size and rheological parameters remained similar to control. In addition, PB-DCA-SA microcapsules showed good excipients’ compatibilities, which were supported by data from differential scanning calorimetry, Fourier transform infrared spectroscopy, scanning electron microscopy, and energy dispersive X-ray studies, suggesting microcapsule stability. Hence, PB-DCA-SA microcapsules have good rheological and compatibility characteristics and may be suitable for the oral delivery of PB in type 2 diabetes.
机译:摘要:作者先前已经设计,开发和表征了一种新型的微囊化制剂,作为一种平台,用于使用普罗布考(PB)药物在2型糖尿病动物模型中靶向治疗。这项研究的目的是通过掺入具有良好渗透增强性能的胆汁酸脱氧胆酸(DCA)来优化PB微胶囊,并研究其对微胶囊的形态,流变性,结构和表面特性以及赋形剂化学成分的影响。和热相容性。微囊化是使用作者实验室中建立的基于BüCHI的微囊化系统进行的。使用聚合物海藻酸钠(SA),制备了两种微囊化制剂:PB-SA(对照)和PB-DCA-SA(测试),其比例保持恒定(分别为1:30和1:3:30)。进行了微囊的完全表征。掺入DCA可获得更好的结构和表面特性,均匀的形态以及稳定的化学和热学曲线,而尺寸和流变参数仍与对照相似。此外,PB-DCA-SA微胶囊具有良好的赋形剂相容性,差示扫描量热法,傅立叶变换红外光谱,扫描电子显微镜和能量色散X射线研究数据支持了PB-DCA-SA的微囊稳定性,表明微胶囊的稳定性。因此,PB-DCA-SA微胶囊具有良好的流变学和相容性特征,并且可能适用于2型糖尿病患者口服PB。

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