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Evaluation of Drug Release Profile from Patches Based on Styrene–Isoprene–Styrene Block Copolymer: The Effect of Block Structure and Plasticizer

机译:基于苯乙烯-异戊二烯-苯乙烯嵌段共聚物的贴剂药物释放曲线评估:嵌段结构和增塑剂的影响

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摘要

We prepared pressure-sensitive adhesive (PSA) patches based on styrene–isoprene–styrene (SIS) thermoplastic elastomer using hot-melt coating method. The liquid paraffine is added in the PSA matrices as a plasticizer to moderate the PSA properties. Three drugs, methyl salicylate, capsaicin, and diphenhydramine hydrochloride are selected as model drugs. The Fourier transform infrared spectroscopy, differential scanning calorimetry test, and wide-angle X-ray diffraction test indicate a good compatibility between drugs and matrices. Peppas equation is used to describe drug release profile. Different drug–matrix absorption, as indicative of drug–matrix interaction, accounts for the variation in release profiles of different drugs. Furthermore, atomic force microscopy and rheological studies of the PSA samples are performed to investigate the effect of SIS structure and plasticizer of PSA on drug release behaviors. For methyl salicylate and capsaicin, drug diffusion in the PSA matrices is the main factor controlled by the release kinetic constant k. The high [SI] diblock content and high plasticizer amount in matrix provide the PSA with a homogeneous and soften microstructure, resulting in a high diffusion rate. But for water-soluble drugs such as diphenhydramine hydrochloride, the release rate is governed by water penetration with the competition from diffusion mechanisms.
机译:我们使用热熔涂布法制备了基于苯乙烯-异戊二烯-苯乙烯(SIS)热塑性弹性体的压敏胶(PSA)贴剂。将液态石蜡作为增塑剂添加到PSA基质中,以调节PSA性能。选择三种药物:水杨酸甲酯,辣椒素和盐酸苯海拉明作为模型药物。傅里叶变换红外光谱,差示扫描量热法测试和广角X射线衍射测试表明药物与基质之间具有良好的相容性。 Peppas方程用于描述药物释放曲线。药物-基质相互作用的不同代表了药物-基质吸收的不同,这解释了不同药物释放曲线的变化。此外,进行了原子力显微镜和PSA样品的流变学研究,以研究SIS结构和PSA增塑剂对药物释放行为的影响。对于水杨酸甲酯和辣椒素,药物在PSA基质中的扩散是释放动力学常数k控制的主要因素。基体中较高的[SI]二嵌段含量和较高的增塑剂含量为PSA提供了均匀且软化的微观结构,从而导致了较高的扩散速率。但是对于水溶性药物,例如盐酸苯海拉明,其释放速率取决于水的渗透以及扩散机制的竞争。

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