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首页> 外文期刊>Nature reviews neuroscience >PBPK Absorption Modeling of Food Effect and Bioequivalence in Fed State for Two Formulations with Crystalline and Amorphous Forms of BCS 2 Class Drug in Generic Drug Development
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PBPK Absorption Modeling of Food Effect and Bioequivalence in Fed State for Two Formulations with Crystalline and Amorphous Forms of BCS 2 Class Drug in Generic Drug Development

机译:在通用药物开发中具有结晶和无定形形式的两种配方的喂养状态的食物效果和生物等效性的PBPK吸收建模

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摘要

Prediction of the effect of food on drug's pharmacokinetics using modeling and simulation could cause difficulties due to complex in vivo processes. A generic formulation with amorphous form of BCS 2 class drug substance was developed and compared in vitro and in vivo to the reference drug product with drug substance in crystalline form. In order to approve generic formulation, some regulatory agencies are requesting to perform bioequivalence (BE) studies also in fed state. Food can have various effects on drug dissolution and absorption, depending also on drug's properties. A physiologically based pharmacokinetic (PBPK) absorption model was built in GastroPlus to predict the food effect on generic and reference formulation and to predict the fed BE study outcome. During model development, we were searching for model inputs that impact and describe in vivo behavior of amorphous and crystalline forms of active pharmaceutical ingredient (API) in fast and fed conditions. The developed model was able to predict the food effect with up to 10% prediction error (PE). Performed virtual BE trials confirmed the BE of drug products in fed state. Our model was able to capture the difference between the two drug products containing different forms of API (amorphous and crystalline) and predict the food effect on both formulations.
机译:使用建模和模拟预测食物对药物药代动力学的影响可能导致体内过程中复杂的困难。通过BCS 2类药物的无定形形式的一种通用配方,并在体外和体内与结晶形式的药物物质进行比较。为了批准普通制定,一些监管机构正在要求在美联储国家进行生物等效性(BE)研究。食物可以对药物溶解和吸收有各种影响,取决于药物的性质。基于生理基础的药代动力学(PBPK)吸收模型内置于腹状,以预测对通用和参考制剂的食物效应并预测美联储的研究结果。在模型开发期间,我们在快速和喂养的条件下搜索了模型输入,该输入会影响无定形和结晶形式的活性药物成分(API)的体内行为。开发的模型能够预测最多10%的预测误差(PE)的食物效果。表演虚拟是试验证实了美联储的药品。我们的模型能够捕捉含有不同形式的API(无定形和结晶)的药物之间的差异,并预测两种制剂的食物效果。

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