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皮质甾类溶解度和脂质极性控制固体脂质纳米粒的释放。

Corticosteroid solubility and lipid polarity control release from solid lipid nanoparticles.

机构信息

LEO Pharma A/S, Industriparken 55, DK-2750 Ballerup, Denmark.

出版信息

Int J Pharm. 2010 May 5;390(1):53-60. doi: 10.1016/j.ijpharm.2009.10.022. Epub 2009 Oct 25.

Abstract

Solid lipid nanoparticles (SLN) show promise as a drug delivery system for skin administration. The solid state of the lipid particle enables efficient drug encapsulation and controlled drug release. The present study addresses the influence of lipid composition and drug substance lipid solubility on the in vitro release profile of corticosteroids from SLN for topical administration. Firstly, the effect of lipid composition on the lipid solubility and in vitro release of betamethasone-17-valerate (BMV) was determined by varying the lipid monoglyceride content and the chain length of the fatty acid moiety. Secondly, the effect of drug substance physicochemical properties was determined by studying five different corticosteroid derivatives with different lipophilicity. A high concentration of monoglyceride in SLN increased the amount of BMV released. The corticosteroid release rate depended on the drug substance lipophilicity and it was clear that the release profiles depended on drug partitioning to the aqueous phase as indicated by zero order kinetics. The results emphasize that the corticosteroid solubility in the lipid phase greatly influence drug distribution in the lipid particles and release properties. Thus knowledge of drug substance solubility and lipid polarity contributes to optimize SLN release properties.

摘要

固体脂质纳米粒 (SLN) 作为经皮给药的药物传递系统具有很大的应用前景。脂质颗粒的固态能够实现高效的药物包封和药物的控制释放。本研究旨在探讨脂质组成和药物脂溶性对 SLN 中皮质甾类药物经皮给药时体外释放特征的影响。首先,通过改变单甘油脂的含量和脂肪酸部分的链长来确定脂质组成对倍他米松-17-戊酸(BMV)的脂溶性和体外释放的影响。其次,通过研究五种不同脂溶性的皮质甾类药物衍生物来确定药物物理化学性质的影响。SLN 中高浓度的单甘油脂会增加 BMV 的释放量。皮质甾类药物的释放速率取决于药物的脂溶性,很明显,释放特征取决于药物向水相的分配,这由零级动力学表明。结果强调了皮质甾类药物在脂质相中的溶解度极大地影响了药物在脂质颗粒中的分布和释放特性。因此,药物物质溶解度和脂质极性的知识有助于优化 SLN 的释放特性。

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