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Liposomes for Enhanced Bioavailability of Water-Insoluble Drugs: In Vivo Evidence and Recent Approaches

机译:脂质体增强水不溶性药物的生物利用度:体内证据和最新方法

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摘要

It has been known that a considerable number of drugs in clinical use or under development are water-insoluble drugs with poor bioavailability (BA). The liposomal delivery system has drawn attention as one of the noteworthy approaches to increase dissolution and subsequently absorption in the gastrointestinal (GI) tract because of its biocompatibility and ability to encapsulate hydrophobic molecules in the lipid domain. However, there have been several drawbacks, such as structural instability in the GI tract and poor permeability across intestinal epithelia because of its relatively large size. In addition, there have been no liposomal formulations approved for oral use to date, despite the success of parenteral liposomes. Nevertheless, liposomal oral delivery has resurged with the rapid increase of published studies in the last decade. However, it is discouraging that most of this research has been in vitro studies only and there have not been many water-insoluble drugs with in vivo data. The present review focused on the in vivo evidence for the improved BA of water-insoluble drugs using liposomes to resolve doubts raised concerning liposomal oral delivery and attempted to provide insight by highlighting the approaches used for in vivo achievements.
机译:众所周知,临床上或开发中的许多药物是生物利用度(BA)差的水不溶性药物。由于脂质体的生物相容性和将疏水性分子包裹在脂质结构域中的能力,脂质体递送系统作为增加溶解度和随后在胃肠道(GI)吸收的值得注意的方法之一而受到关注。然而,存在一些缺点,例如由于其相对大的尺寸,所以胃肠道中的结构不稳定性以及肠上皮的通透性差。另外,尽管肠胃外脂质体成功,但迄今尚无批准用于口服的脂质体制剂。然而,随着近十年来发表的研究的迅速增加,脂质体的口服递送已经减少。然而,令人沮丧的是,大多数研究仅是体外研究,并且没有许多具有体内数据的水不溶性药物。本综述集中在体内证据,该研究使用脂质体改善了水不溶性药物的BA,以解决有关脂质体口服给药的疑问,并试图通过强调用于体内成就的方法来提供见解。

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