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Mechanically Robust Gastroretentive Drug-Delivery Systems Capable of Controlling Dissolution Behaviors of Coground β-Lapachone

机译:机械鲁棒的胃滞留药物输送系统能够控制共研磨的β-拉帕酮的溶解行为

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摘要

In this study, we aimed to design a highly swellable and mechanically robust matrix tablet (SMT) as a gastroretentive drug-delivery system (GRDDS) capable of improving the dissolution behavior of β-lapachone with low aqueous solubility. For the preparation of SMTs, the cogrinding technique and freeze–thaw method were used to disperse β-lapachone in SMTs in an amorphous state and to enhance the swelling and mechanical properties of SMTs, respectively. As a result, the crystallinity of coground β-lapachone incorporated in the SMTs was found to be considerably decreased; thereby, the dissolution rates of the drug in a simulated gastric fluid could be substantially increased. The SMTs of β-lapachone also demonstrated significantly enhanced swelling and mechanical properties compared to those of a marketed product. The reason for this might be because the physically crosslinked polymeric networks with a porous structure that were formed in SMTs through the freeze–thaw method. In addition, β-lapachone was gradually released from the SMTs in 6 h. Therefore, SMTs of β-lapachone developed in this study could be used as GRDDS with appropriate swelling and mechanical properties for improving the dissolution behavior of hydrophobic drugs such as β-lapachone.
机译:在这项研究中,我们旨在设计一种高度溶胀和机械坚固的基质片剂(SMT),作为一种胃滞留性药物传递系统(GRDDS),能够改善低水溶性的β-拉帕酮的溶解行为。为了制备SMT,使用共研磨技术和冻融法将β-拉帕酮以无定形状态分散在SMT中,并分别增强SMT的溶胀和机械性能。结果,发现掺入SMT中的共研磨的β-拉帕酮的结晶度显着降低。因此,可以大大提高药物在模拟胃液中的溶解速率。与市售产品相比,β-lapachone的SMT也显示出明显增强的溶胀和机械性能。其原因可能是因为通过冻融法在SMT中形成的具有多孔结构的物理交联聚合物网络。此外,β-拉帕酮在6小时内逐渐从SMT中释放出来。因此,本研究开发的β-拉帕酮表面活性剂可用作具有良好溶胀和力学性能的GRDDS,可改善疏水性药物(例如β-拉帕酮)的溶解行为。

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