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Ibuprofen nanocrystals developed by 2 2 factorial design experiment: A new approach for poorly water-soluble drugs

机译:通过2 2析因设计实验开发的布洛芬纳米晶体:水溶性差的药物的新方法

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The reduction of the particle size of drugs of pharmaceutical interest down to the nano-sized range has dramatically changed their physicochemical properties. The greatest disadvantage of nanocrystals is their inherent instability, due to the risk of crystal growth. Thus, the selection of an appropriate stabilizer is crucial to obtain long-term physicochemically stable nanocrystals. High pressure homogenization has enormous advantages, including the possibility of scaling up, lack of organic solvents and the production of small particles diameter with low polydispersity index. The sequential use of high shear homogenization followed by high pressure homogenization, can modulate nanoparticles’ size for different administration routes. The present study focuses on the optimization of the production process of two formulations composed of different surfactants produced by High Shear Homogenization followed by hot High Pressure Homogenization. To build up the surface response charts, a 22 full factorial design experiment, based on 2 independent variables, was used to develop optimized formulations. The effects of the production process on the mean particle size and polydispersity index were evaluated. The best ibuprofen nanocrystal formulations were obtained using 0.20% Tween 80 and 1.20% PVP K30 (F1) and 0.20% Tween 80 and 1.20% Span 80 (F2). The estimation of the long-term stability of the aqueous suspensions of ibuprofen nanocrystals was studied using the LUMISizer. The calculated instability index suggests that F1 was more stable when stored at 4 °C and 22 °C, whereas F2 was shown to be more stable when freshly prepared.
机译:将药用药物的粒径减小至纳米级范围已极大地改变了其理化性质。纳米晶体的最大缺点是由于晶体生长的风险,其固有的不稳定性。因此,选择合适的稳定剂对于获得长期的物理化学稳定的纳米晶体至关重要。高压均质化具有巨大的优势,包括可能扩大规模,缺少有机溶剂以及生产具有低多分散指数的小粒径。先后使用高剪切均质化和高压均质化,可以调节纳米颗粒的大小,以适应不同的给药途径。本研究着重优化由高剪切均质化然后热高压均质化生产的两种由不同表面活性剂组成的配方的生产工艺。为了建立表面响应图,基于22个独立变量的22个全因子设计实验用于开发优化配方。评估了生产工艺对平均粒径和多分散指数的影响。使用0.20%的Tween 80和1.20%的PVP K30(F1)和0.20%的Tween 80和1.20%的Span 80(F2)可获得最佳的布洛芬纳米晶体配方。使用LUMISizer研究了布洛芬纳米晶体水悬浮液的长期稳定性估计。计算出的不稳定性指数表明,F1在4°C和22°C下储存时更稳定,而F2在新鲜制备时更稳定。

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