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Preparation and in vitro release kinetics of ivermectin sustained-release bolus optimized by response surface methodology

机译:响应面法优化伊维菌素缓释丸的制备及体外释放动力学

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摘要

Sustained-release formulations of ivermectin (IVM) are useful for controlling parasitic diseases in animals. In this work, an IVM bolus made from microcrystalline cellulose (MCC), starch and low-substituted hydroxypropyl cellulose (LS-HPC) was optimized by response surface methodology. The bolus was dissolved in a cup containing 900 mL of dissolution medium at 39.5 °C, under with stirring at 100 rpm. A quadratic model was formulated using analysis of variance according to the dissolution time. The optimized formulation of the bolus contained 8% MCC, 0.5% starch, and 0.25% LS-HPC. The length, width, and height of the prepared IVM bolus were 28.12 ± 0.14, 16.1 ± 0.13, and 13.03 ± 0.05 mm, respectively. The bolus weighed 11.4842 ± 0.1675 g (with a density of 1.95 g/cm3) and contained 458.26 ± 6.68 mg of IVM. It exhibited in vitro sustained-release for over 60 days, with a cumulative amount and percentage of released IVM of 423.72 ± 5.48 mg and 92.52 ± 1.20%, respectively. The Korsmeyer–Peppas model provided the best fit to the dissolution release kinetics, exhibiting an R2 value close to 1 and the lowest Akaike Information Criterion among different models. The parameter n (0.5180) of the Korsmeyer–Peppas model was between 0.45 and 0.89. It was demonstrated that the release mechanism of the IVM bolus followed a diffusive erosion style.
机译:伊维菌素(IVM)的缓释制剂可用于控制动物的寄生虫病。在这项工作中,通过响应表面方法优化了由微晶纤维素(MCC),淀粉和低取代羟丙基纤维素(LS-HPC)制成的IVM推注。将大丸剂在100rpm搅拌下在39.5℃下溶解于装有900mL溶解介质的杯子中。根据溶解时间使用方差分析来制定二次模型。药丸的优化配方包含8%MCC,0.5%淀粉和0.25%LS-HPC。制备的IVM推注的长度,宽度和高度分别为28.12±0.14、16.1±0.13和13.03±0.05 mm。弹丸重11.4842±0.1675 g(密度为1.95 g / cm 3 ),并含458.26±6.68 mg IVM。它在体外持续释放超过60天,累计IVM的累积量和释放百分比分别为423.72±5.48 mg和92.52±1.20%。 Korsmeyer-Peppas模型最适合溶出释放动力学,在不同模型中显示的R 2 值接近1,最低的Akaike信息准则。 Korsmeyer-Peppas模型的参数n(0.5180)在0.45和0.89之间。事实证明,IVM推注的释放机制遵循扩散性侵蚀形式。

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