首页> 外文期刊>International Journal of Pharmaceutics >Use of compressed gas precipitation to enhance the dissolution behavior of a poorly water-soluble drug: generation of drug microparticles and drug-polymer solid dispersions.
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Use of compressed gas precipitation to enhance the dissolution behavior of a poorly water-soluble drug: generation of drug microparticles and drug-polymer solid dispersions.

机译:使用压缩气体沉淀来增强水溶性差的药物的溶解行为:药物微粒和药物聚合物固体分散体的产生。

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摘要

The classical anticonvulsant drug phenytoin (5,5-diphenyl hydantoin, C(15)H(12)N(2)O(2)) has been used as a model compound to investigate the possibility of enhancing the dissolution rate of poorly water-soluble drugs using dense gas antisolvent techniques. In a first step, microcrystals of neat phenytoin have been generated using the gas antisolvent (GAS) and precipitation with compressed antisolvent (PCA) processes, thereby assessing process performances and elucidating similarities and differences between the two techniques. In a second step, the PCA process has been used to generate solid dispersions of phenytoin in the hydrophilic polymer poly(vinyl-pyrrolidone)-K30 (PVP). In vitro dissolution results reveal a substantially better performance of the PCA-processed co-formulations compared to unprocessed phenytoin and to GAS- and PCA-precipitates of neat drug crystals. A comparison of the product quality of phenytoin-PVP co-formulations with solid dispersions obtained by spray drying convincingly underlines the potential of dense gas antisolvent techniques for the production of pharmaceutical formulations with enhanced oral bioavailability.
机译:经典的抗惊厥药苯妥英钠(5,5-二苯基乙内酰脲,C(15)H(12)N(2)O(2))已用作模型化合物,以研究提高不良水的溶解速率的可能性。溶解性药物使用重气抗溶剂技术。第一步,使用气体抗溶剂(GAS)和压缩抗溶剂(PCA)沉淀法生成了纯苯妥英钠微晶,从而评估了工艺性能并阐明了两种技术之间的异同。在第二步中,已使用PCA工艺在亲水性聚合物聚(乙烯基-吡咯烷酮)-K30(PVP)中生成苯妥英钠的固体分散体。体外溶出结果表明,与未加工的苯妥英钠以及纯药物晶体的GAS和PCA沉淀物相比,PCA处理的共制剂的性能要好得多。将苯妥英-PVP共制剂与通过喷雾干燥获得的固体分散体的产品质量进行比较,令人信服地强调了致密气体反溶剂技术在生产口服生物利用度提高的药物制剂方面的潜力。

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