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自组装纳米结构液晶颗粒作为孕酮经皮递送的一种有前景的载体。

Self-assembled nano-architecture liquid crystalline particles as a promising carrier for progesterone transdermal delivery.

作者信息

Elgindy Nazik A, Mehanna Mohammed M, Mohyeldin Salma M

机构信息

Department of Industrial Pharmacy, Faculty of Pharmacy, Alexandria University, Alexandria, Egypt.

Department of Industrial Pharmacy, Faculty of Pharmacy, Alexandria University, Alexandria, Egypt; Department of Pharmaceutical Technology, Faculty of Pharmacy, Beirut Arab University, Beirut, Lebanon.

出版信息

Int J Pharm. 2016 Mar 30;501(1-2):167-79. doi: 10.1016/j.ijpharm.2016.01.049. Epub 2016 Jan 29.

Abstract

The study aims to elaborate novel self-assembled liquid crystalline nanoparticles (LCNPs) for management of hormonal disturbances following non-invasive progesterone transdermal delivery. Fabrication and optimization of progesteroneloaded LCNPs for transdermal delivery were assessed via a quality by design approach based on 2(3) full factorial design. The design includes the functional relationships between independent processing variables and dependent responses of particle size, polydispersity index, zeta potential, cumulative drug released after 24h and ex-vivo transdermal steady flux. The developed nanocarrier was subjected to TEM (transmission electron microscope) for morphological elucidation and stability study within a period of three months at different storage temperatures. The cubic phase of LCNPs was successfully prepared using glyceryl monooleate (GMO) via the emulsification technique. Based on the factorial design, the independent operating variables significantly affected the five dependent responses. The cubosomes hydrodynamic diameters were in the nanometric range (101-386 nm) with narrow particle size distribution, high negative zeta potential ≥-30 mV and entrapment efficiency ≥94%. The LCNPs succeeded in sustaining progesterone release for almost 24h, following a non-fickian transport of drug diffusion mechanism. Ex-vivo study revealed a significant enhancement up to 6 folds in the transdermal permeation of progesterone-loaded LCNPs compared to its aqueous suspension. The optimized LCNPs exhibited a high physical stability while retaining the cubic structure for at least three months. Quality by design approach successfully accomplished a predictable mathematical model permitting the development of novel LCNPs for transdermal delivery of progesterone with the benefit of reducing its oral route side effects.

摘要

本研究旨在制备新型自组装液晶纳米颗粒(LCNPs),用于无创经皮递送孕酮后激素紊乱的管理。通过基于2(3)全因子设计的质量源于设计方法,评估了用于经皮递送的载孕酮LCNPs的制备和优化。该设计包括独立加工变量与粒径、多分散指数、zeta电位、24小时后累积药物释放量和离体经皮稳定通量等相关响应之间的函数关系。对所制备的纳米载体进行透射电子显微镜(TEM)分析,以阐明其形态,并在不同储存温度下进行为期三个月的稳定性研究。通过乳化技术,使用单油酸甘油酯(GMO)成功制备了LCNPs的立方相。基于因子设计,独立操作变量对五个相关响应有显著影响。立方液晶纳米粒的流体动力学直径在纳米范围内(101-386 nm),粒径分布窄,zeta电位高且为负≥-30 mV,包封率≥94%。LCNPs成功实现了孕酮近24小时的持续释放,遵循非菲克扩散机制的药物扩散。离体研究表明,与水性悬浮液相比,载孕酮LCNPs的经皮渗透显著提高了6倍。优化后的LCNPs表现出高物理稳定性,同时至少三个月保持立方结构。质量源于设计方法成功建立了一个可预测的数学模型,有助于开发用于经皮递送孕酮的新型LCNPs,减少其口服途径的副作用。

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