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首页> 外文期刊>Drug development and industrial pharmacy >Process and formulation variables affecting the performance of a rupturable capsule-based drug delivery system with pulsatile drug release.
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Process and formulation variables affecting the performance of a rupturable capsule-based drug delivery system with pulsatile drug release.

机译:工艺和配方变量会影响具有脉冲性药物释放的基于可破裂胶囊的药物输送系统的性能。

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摘要

The objective of this study was to optimize several process and formulation parameters, which influence the performance of a rupturable, pulsatile drug delivery system. The system consisted of a drug-containing hard gelatin capsule, a swelling layer of croscarmellose (Ac-Di-Sol) and a binder, and an outer ethylcellulose coating. Polyvinyl pyrrolidone (Kollidon 90F) was superior to HPMC and HPC as a binder for the swelling layer with regard to binding (adherence to capsule) and disintegration properties of the swelling layer. The capsule-to-capsule uniformity in the amount of swelling layer and outer ethylcellulose coating, which significantly affected the lag time prior to rupture of the capsule, was optimized by decreasing the batch size, and by increasing the rotational pan speed and the distance between the spray nozzle and the product bed. The type of baffles used in the coating pan also affected the layering uniformity. Fully-filled hard gelatin capsules had a shorter lag time with a higher reproducibility compared to only half-filled capsules, because the swelling pressure was directed primarily to the outer ethylcellulose coating and not to the inner capsule core. Stability studies revealed that the lag time of the capsules was stable over a 240-day period when the moisture content was kept unchanged.
机译:这项研究的目的是优化一些工艺和配方参数,这些参数会影响可破裂的搏动性药物输送系统的性能。该系统由含药物的硬明胶胶囊,交联羧甲基纤维素(Ac-Di-Sol)和粘合剂的溶胀层以及乙基纤维素外涂层组成。聚乙烯吡咯烷酮(Kollidon 90F)作为溶胀层的粘合剂,在溶胀层的粘合(对胶囊的粘附)和崩解性能方面优于HPMC和HPC。通过减小批次大小,增加旋转锅速度和之间的距离,可以优化溶胀层和乙基乙基纤维素外层的数量,从而显着影响胶囊破裂之前的滞后时间,从而优化了胶囊之间的均匀性喷嘴和产品床。涂层锅中使用的挡板的类型也影响分层的均匀性。与仅半填充的胶囊相比,完全填充的硬明胶胶囊具有较短的延迟时间和较高的重现性,因为溶胀压力主要指向外部乙基纤维素包衣而不是内部胶囊芯。稳定性研究表明,当水分含量保持不变时,胶囊的滞后时间在240天的时间内是稳定的。

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