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利用脂质增强药物吸收:一项案例研究,介绍一种用于治疗全身性真菌感染的新型脂质体两性霉素B口服制剂的研发及药理学评价。

Enhancing drug absorption using lipids: a case study presenting the development and pharmacological evaluation of a novel lipid-based oral amphotericin B formulation for the treatment of systemic fungal infections.

作者信息

Sachs-Barrable Kristina, Lee Stephen D, Wasan Ellen K, Thornton Sheila J, Wasan Kishor M

机构信息

Faculty of Pharmaceutical Sciences, University of British Columbia, Vancouver, BC, Canada V6T 1Z3.

出版信息

Adv Drug Deliv Rev. 2008 Mar 17;60(6):692-701. doi: 10.1016/j.addr.2007.08.042. Epub 2007 Nov 5.

Abstract

The development of a safe and efficacious drug involves a balance between bioavailability, toxicity and disposition within the body. If the drug is hydrophobic or acid labile, oral administration may lead to poor systemic exposure, necessitating a parenteral treatment regime. Amphotericin B (AmpB) is one example of a well established, highly efficacious drug that has a 50 year history of intravenous therapy. AmpB formulated as a micellar dispersion (Fungizone; FZ) for IV use, remains one of the most effective agents in the treatment of systemic fungal infections, yet no oral formulations are currently commercially available. Recently, our laboratory has developed new oral lipid-based AmpB formulations with enhanced gastrointestinal (GI) tract absorption and antifungal activity with minimum renal toxicity. This review article will discuss these findings and present data to support two potential mechanisms for the enhanced GI tract absorption of AmpB when formulated in this oral lipid-based delivery system, namely an increase in lymphatic drug transport and a decrease in pre-systemic transporter-mediated drug efflux.

摘要

一种安全有效的药物的研发涉及生物利用度、毒性和体内处置之间的平衡。如果药物具有疏水性或酸不稳定性,口服给药可能导致全身暴露不佳,因此需要采用肠胃外治疗方案。两性霉素B(AmpB)是一种成熟的高效药物,已有50年的静脉治疗历史,它就是一个例子。以胶束分散体(两性霉素B注射剂;FZ)形式配制用于静脉注射的AmpB,仍然是治疗系统性真菌感染最有效的药物之一,但目前尚无口服制剂上市。最近,我们实验室开发了新的基于脂质的口服AmpB制剂,具有增强的胃肠道(GI)吸收和抗真菌活性,且肾毒性最小。这篇综述文章将讨论这些发现,并提供数据支持在这种基于脂质的口服给药系统中配制AmpB时增强胃肠道吸收的两种潜在机制,即淋巴药物转运增加和系统前转运体介导的药物外排减少。

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