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用于增强药代动力学性能的阿瑞匹坦口腔崩解膜的研发。

Development of aprepitant loaded orally disintegrating films for enhanced pharmacokinetic performance.

作者信息

Sharma Radhika, Kamboj Sunil, Singh Gursharan, Rana Vikas

机构信息

Pharmaceutics Division, Dept. of Pharmaceutical Sciences and Drug Research, Punjabi University, Patiala 147002, India.

Pharmaceutics Division, Dept. of Pharmaceutical Sciences and Drug Research, Punjabi University, Patiala 147002, India.

出版信息

Eur J Pharm Sci. 2016 Mar 10;84:55-69. doi: 10.1016/j.ejps.2016.01.006. Epub 2016 Jan 9.

Abstract

The present investigation was aimed to prepare orally disintegrating films (ODFs) containing aprepitant (APT), an antiemetic drug employing pullulan as film forming agent, tamarind pectin as wetting agent and liquid glucose as plasticizer and solubiliser. The ODFs were prepared using solvent casting method. The method was optimized employing 3(2) full factorial design considering proportion of pullulan: tamarind pectin and concentration of liquid glucose as independent variables and disintegration time, wetting time, folding endurance, tensile strength and extensibility as dependent variables. The optimized ODF was evaluated for various physicochemical, mechanical, drug release kinetics and bioavailability studies. The results suggested prepared film has uniform film surface, non-sticky and disintegrated within 18s. The in-vitro release kinetics revealed more than 87% aprepitant was released from optimized ODF as compared to 85%, 49%, and 12% aprepitant release from marketed formulation Aprecap, micronized aprepitant and non micronized aprepitant, respectively. The results of animal preference study indicated that developed aprepitant loaded ODFs are accepted by rabbits as food material. Animal pharmacokinetic (PK) study showed 1.80, 1.56 and 1.36 fold enhancement in relative bioavailability for aprepitant loaded ODF, Aprecap and micronized aprepitant respectively, in comparison with non-micronized aprepitant. Overall, the solubilised aprepitant when incorporated in the form of aprepitant loaded ODF showed enhanced bioavailability as compared to micronized/non-micronized aprepitant based oral formulations. These findings suggested that aprepitant loaded ODF could be effective for antiemesis during cancer chemotherapy.

摘要

本研究旨在制备含阿瑞匹坦(APT)的口腔崩解膜(ODF),阿瑞匹坦是一种止吐药,采用普鲁兰多糖作为成膜剂,罗望子果胶作为湿润剂,液体葡萄糖作为增塑剂和增溶剂。采用溶剂浇铸法制备ODF。该方法采用3(2)全因子设计进行优化,将普鲁兰多糖与罗望子果胶的比例和液体葡萄糖的浓度作为自变量,崩解时间、湿润时间、耐折性、拉伸强度和延展性作为因变量。对优化后的ODF进行了各种物理化学、机械、药物释放动力学和生物利用度研究。结果表明,制备的膜表面均匀,不粘腻,在18秒内崩解。体外释放动力学显示,与市售制剂Aprecap、微粉化阿瑞匹坦和非微粉化阿瑞匹坦分别释放85%、49%和12%的阿瑞匹坦相比,优化后的ODF释放的阿瑞匹坦超过87%。动物偏好性研究结果表明,所开发的载阿瑞匹坦ODF被兔子作为食物材料所接受。动物药代动力学(PK)研究表明,与非微粉化阿瑞匹坦相比,载阿瑞匹坦ODF、Aprecap和微粉化阿瑞匹坦的相对生物利用度分别提高了1.80倍、1.56倍和1.36倍。总体而言,与基于微粉化/非微粉化阿瑞匹坦的口服制剂相比,以载阿瑞匹坦ODF形式掺入的增溶阿瑞匹坦显示出更高的生物利用度。这些发现表明,载阿瑞匹坦ODF可能对癌症化疗期间的止吐有效。

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