Preparation, characterization and scale-up of sesamol loaded solid lipid nanoparticles

Vandita Kakkar, I. Kaur
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引用次数: 13

Abstract

Sesamol loaded solid lipid nanoparticles (SSLNs) were prepared with the aim of minimizing its distribution to tissues and achieving its targeting to the brain. Three scale-up batches (100x1 L) of S-SLNs were prepared using a microemulsification technique and all parameters were statistically compared with the small batch (1x;10 mL). S-SLNs with a particle size of less than 106 nm with a spherical shape (transmission electron microscopy) were successfully prepared with a total drug content and entrapment efficiency of 94.26±2.71% and 72.57±5.20%, respectively. Differential scanning calorimetry and infrared spectroscopy confirmed the formation of lipidic nanoparticles while powder X-ray diffraction revealed their amorphous profile. S-SLNs were found to be stable for three months at 5±3°C in accordance with International Conference on Harmonisation guidelines. The SLN preparation process was successfully scaled-up to a 100x batch on a laboratory scale. The procedure was easy to perform and allowed reproducible SLN dispersions to be obtained.
芝麻酚负载固体脂质纳米颗粒的制备、表征和规模化研究
制备了芝麻酚负载的固体脂质纳米颗粒(ssln),目的是尽量减少其在组织中的分布,并实现其对大脑的靶向。采用微乳化技术制备了3个放大批次(100x1 L)的s - sln,并将所有参数与小批次(1x;10 mL)进行统计学比较。成功制备了粒径小于106 nm的球形S-SLNs(透射电镜),总药物含量和包封效率分别为94.26±2.71%和72.57±5.20%。差示扫描量热法和红外光谱法证实了脂质纳米颗粒的形成,而粉末x射线衍射显示了它们的无定形轮廓。根据国际协调会议的指导方针,发现s - sln在5±3°C下稳定三个月。SLN制备工艺在实验室规模上成功地扩大到100倍批次。该方法操作简单,可获得可重复的SLN分散体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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