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多孔载体固体自微乳药物传递系统的特性评价及其作为改善卡马西平释放的系统。

Characterization and evaluation of solid self-microemulsifying drug delivery systems with porous carriers as systems for improved carbamazepine release.

机构信息

Department of Pharmaceutical Technology and Cosmetology, University of Belgrade, Faculty of Pharmacy, Vojvode Stepe 450, P.O. Box 146, 11221 Belgrade, Serbia.

出版信息

Int J Pharm. 2012 Oct 15;436(1-2):58-65. doi: 10.1016/j.ijpharm.2012.06.032. Epub 2012 Jun 18.

Abstract

The purpose of this study was to investigate solid self-microemulsifying drug delivery system (SSMEDDS), as potential delivery system for poorly water soluble drug carbamazepine (CBZ). Self-microemulsifying drug delivery system (SMEDDS) was formulated using the surfactant polyoxyethylene 20 sorbitan monooleate [Polysorbate 80] (S), the cosurfactant PEG-40 hydrogenated castor oil [Cremophor(®) RH40] (C) and the oil caprylic/capric triglycerides [Mygliol(®) 812] (O). Four different adsorbents with high specific surface area were used: Neusilin(®) UFL2, Neusilin(®) FL2 (magnesium aluminometasilicate), Sylysia(®) 320 and Sylysia(®) 350 (porous silica). Microemulsion area at the surfactant to cosurfactant ratio (K(m)) 1:1 was evaluated and for further investigation SMEDDS with SC/O ratio 8:2 was selected. Solubilization capacity of selected SMEDDS for CBZ was 33.771±0.041 mg/ml. Rheological measurements of unloaded and CBZ-loaded SMEDDS at water content varied from 10 to 60% (w/w) were conducted. It has been found that CBZ has great influence on rheological behaviour of investigated system upon water dilution. Photon correlation spectroscopy has shown the ability of CBZ-loaded SMEDDS to produce microemulsion droplet size. SSMEDDS improved release rate of CBZ, but the type of adsorbent significantly affects release rate of CBZ. For SSMEDDS with different magnesium aluminometasilicate adsorbents, release rate of CBZ decreased with increasing specific surface area due to entrapment of liquid SMEDDS inside the pores and its gradual exposure to dissolution medium. With porous silica adsorbents no difference in release rate was found in comparison to physical mixtures. In physical mixtures at 12.5% (w/w) CBZ content, presence of amorphous CBZ led to high dissolution rate.

摘要

本研究旨在探讨固体自微乳药物传递系统(SSMEDDS)作为难溶性药物卡马西平(CBZ)的潜在传递系统。自微乳药物传递系统(SMEDDS)是使用表面活性剂聚氧乙烯 20 山梨醇单油酸酯[聚山梨酯 80](S)、助表面活性剂聚乙二醇 40 氢化蓖麻油[Cremophor(®)RH40](C)和油辛酸/癸酸三甘油酯[Mygliol(®)812](O)制成的。使用了四种具有高比表面积的不同吸附剂:Neusilin(®)UFL2、Neusilin(®)FL2(硅酸镁铝)、Sylysia(®)320 和 Sylysia(®)350(多孔硅)。评估了表面活性剂与助表面活性剂比例(K(m))为 1:1 的微乳液区域,并且为了进一步研究,选择了 SC/O 比为 8:2 的 SMEDDS。选定的 SMEDDS 对 CBZ 的增溶能力为 33.771±0.041mg/ml。在水含量从 10%至 60%(w/w)变化的情况下,对未加载和加载 CBZ 的 SMEDDS 进行了流变测量。研究发现,CBZ 对水稀释时研究体系的流变行为有很大影响。光子相关光谱法表明,载有 CBZ 的 SMEDDS 具有产生微乳液液滴尺寸的能力。SSMEDDS 提高了 CBZ 的释放速率,但吸附剂的类型显著影响 CBZ 的释放速率。对于具有不同硅酸镁铝吸附剂的 SSMEDDS,CBZ 的释放速率随比表面积的增加而降低,这是由于液体 SMEDDS 被捕获在孔内,并且其逐渐暴露于溶解介质中。与物理混合物相比,使用多孔硅吸附剂时,发现 CBZ 的释放速率没有差异。在物理混合物中,当 CBZ 含量为 12.5%(w/w)时,无定形 CBZ 的存在导致高溶解速率。

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