首页> 外文期刊>Pharmaceutical development and technology >Role of cyclodextrin complexation in felodipine-sustained release matrix tablets intended for oral transmucosal delivery: in vitro and ex vivo characterization.
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Role of cyclodextrin complexation in felodipine-sustained release matrix tablets intended for oral transmucosal delivery: in vitro and ex vivo characterization.

机译:环糊精络合物在非洛地平缓释基质片剂中的作用,旨在口服经粘膜递送:体外和离体表征。

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摘要

The objective of the present research was two-fold: To characterize the produced inclusion complex of felodipine (FDP)-hydroxypropyl-β-cyclodextrin (HPβCD) utilizing lyophilization, and to develop and characterize a complexed sustained-release polymeric matrix tablets intended for buccal delivery. The phase-solubility diagram suggested an A(L) type system with 1:1 stoichiometry. Solid complexes prepared by physical mixing and lyophilization were characterized by thermal and non-thermal analytical techniques to corroborate the fact of complex formation. The sustained-release FDP tablets were produced by direct compression, and these drug or complex-loaded hydrophilic matrices were assessed for in vitro bioadhesion and release modulation, ex vivo permeation, and in vivo residence time. The in vitro drug release and ex vivo permeation across the porcine buccal membrane demonstrated that the matrix tablets containing FDP-HPβCD (FH5) solid complex exhibited a complete and sustained drug release pattern, and a significantly higher drug permeation (p?
机译:本研究的目的有两个方面:利用冻干法表征非洛地平(FDP)-羟丙基-β-环糊精(HPβCD)产生的包合物,并开发和表征用于口腔的复合缓释聚合物基质片剂交货。相溶解度图建议使用化学计量比为1:1的A(L)型系统。通过物理混合和冻干制备的固体复合物通过热和非热分析技术进行表征,以证实复合物形成的事实。通过直接压制生产缓释FDP片剂,并评估这些药物或复合物负载的亲水性基质的体外生物粘附和释放调节,离体渗透和体内停留时间。穿过猪颊膜的体外药物释放和离体渗透表明,含有FDP-HPβCD(FH5)固体复合物的基质片剂表现出完整且持续的药物释放模式,并且药物渗透性显着更高(p 0.05)。与所有其他受测配方相比。这可以归因于FDP-HPβCD络合现象和制剂中亲水性聚合物的存在。所有测试的制剂在人唾液中均表现出良好的稳定性。另外,在健康的人类志愿者中研究了优化制剂的体内粘膜粘附行为,并评估了主观参数。

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