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β-谷甾醇浓度和高压均质化对洗必泰从囊泡凝胶中释放的影响。

Effect of beta-sitosterol concentration and high pressure homogenization on the chlorhexidine release from vesicular gels.

作者信息

Farkas E, Schubert R, Zelkó R

机构信息

Pharmaceutical Institute, Semmelweis University, Hogyes E. Street 7, 1092 Budapest, Hungary.

出版信息

Int J Pharm. 2006 Jan 3;307(1):51-5. doi: 10.1016/j.ijpharm.2005.09.018. Epub 2005 Oct 27.

Abstract

Previous studies have confirmed that the phase transition of vesicular gels of hydrogenated phospholipids to the less ordered fluid vesicular state was induced by the increase of the beta-sitosterol ratio in the whole gel system and consequently in the lipid bilayer. The purpose of the present study was to evaluate the influence of the beta-sitosterol portion in the lipid bilayer and the effect of high pressure homogenization on the structural characteristics of the prepared gel systems. In addition the influence of beta-sitosterol on the consequent chlorhexidine release from the obtained vesicles and liposomes was also examined. Lipid mixtures were prepared from different molar ratios of lecithin:sterol components (90:10-65:35 mol%). The obtained mixtures were hydrated with the aqueous solution of chlorhexidine digluconate in order to achieve a 30% (w/w) final concentration of the lipid mixtures and a 4% (w/w) concentration of the drug. One portion of the resultant multilamellar vesicles was homogenized by using high pressure. To characterize the homogenized and non-homogenized systems, transmission electron microscopy of the freeze-fractured samples and differential scanning calorimetry (DSC) were carried out. A vertical type diffusion cell was applied to determine the amount of released chlorhexidine digluconate. Along with the increase in beta-sitosterol concentration, the fluidity of the membrane as well as its permeability also increased. The increased permeability--caused by the higher beta-sitosterol concentration--and the high pressure homogenization, which increased the dispersity and therefore the surface area, enabled a higher amount of chlorhexidine to be released. The increase of drug release was more pronounced in the case of samples prepared with high pressure homogenization.

摘要

先前的研究已经证实,氢化磷脂的囊泡凝胶向无序程度较低的流体囊泡状态的相变是由整个凝胶系统中β-谷甾醇比例的增加引起的,进而导致脂质双层中该比例增加。本研究的目的是评估脂质双层中β-谷甾醇部分的影响以及高压均质化对所制备凝胶系统结构特征的影响。此外,还研究了β-谷甾醇对所得囊泡和脂质体中洗必泰释放的后续影响。由不同摩尔比的卵磷脂:甾醇成分(90:10 - 65:35摩尔%)制备脂质混合物。将所得混合物用葡萄糖酸氯己定水溶液水合,以达到脂质混合物最终浓度为30%(w/w)和药物浓度为4%(w/w)。所得多层层状囊泡的一部分通过高压进行均质化处理。为了表征均质化和未均质化的系统,对冷冻断裂样品进行了透射电子显微镜检查和差示扫描量热法(DSC)分析。使用垂直型扩散池测定释放的葡萄糖酸氯己定的量。随着β-谷甾醇浓度的增加,膜的流动性及其渗透性也增加。由较高的β-谷甾醇浓度引起的渗透性增加以及高压均质化增加了分散度从而增加了表面积,使得能够释放更多量的洗必泰。在通过高压均质化制备的样品中,药物释放的增加更为明显。

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