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A quality by design (QbD) twin–screw extrusion wet granulation approach for processing water insoluble drugs

机译:设计质量(QbD)双螺杆挤出湿法制粒方法,用于处理水不溶性药物

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摘要

In this study, a Quality by Design (QbD) approach was used to identify the effect of formulation parameters in a twin screw wet extrusion granulation process for the manufacturing of ibuprofen (IBU) granules with increased dissolution rates. A fractional factorial Design of Experiment (DoE) was used to investigate the effect of the excipient composition, binder amount and liquid to solid (L/S) ratio (independent variables) on drug dissolution rates, median particle size diameter and specific surface area (dependent variables). The intra-granular addition of the binder in inorganic/polymer blends processed with ethanol as granulating liquids facilitated the formation of granules at various particle sizes. DoE regression analysis showed that all formulation parameters affect the dependent variables significantly. The enhanced dissolution rates were attributed not only to the IBU particle size reduction and adsorption in the porous inorganic network but also to the high specific surface area of the produced granules. Dynamic vapour sorption showed increased water absorption for granules with small particle size distribution and high specific surface area.
机译:在这项研究中,通过设计质量(QbD)方法来确定制剂参数在双螺杆湿法挤压制粒工艺中对溶解速率提高的布洛芬(IBU)颗粒制造的影响。使用分数阶乘实验设计(DoE)来研究赋形剂组成,粘合剂含量和液固比(L / S)(独立变量)对药物溶出速率,中值粒径和比表面积(因变量)。在用乙醇作为造粒液体处理的无机/聚合物共混物中,在颗粒内添加粘合剂有助于形成各种粒径的颗粒。 DoE回归分析表明,所有配方参数均会显着影响因变量。溶解速率的提高不仅归因于IBU粒径的减小和在多孔无机网络中的吸附,还归因于所生产颗粒的高比表面积。动态蒸气吸附显示出具有较小粒径分布和高比表面积的颗粒的吸水率增加。

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