首页> 美国卫生研究院文献>CPT: Pharmacometrics Systems Pharmacology >Combining Bottom‐up and Top‐down Approaches to Assess the Impact of Food and Gastric pH on Pictilisib (GDC‐0941) Pharmacokinetics
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Combining Bottom‐up and Top‐down Approaches to Assess the Impact of Food and Gastric pH on Pictilisib (GDC‐0941) Pharmacokinetics

机译:结合自下而上和自上而下的方法来评估食品和胃液pH值对Pictilisib的影响(GDC-0941)药代动力学

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摘要

Pictilisib, a weakly basic compound, is an orally administered, potent, and selective pan‐inhibitor of phosphatidylinositol 3‐kinases for oncology indications. To investigate the significance of high‐fat food and gastric pH on pictilisib pharmacokinetics (PK) and enable label recommendations, a dedicated clinical study was conducted in healthy volunteers, whereby both top‐down (population PK, PopPK) and bottom‐up (physiologically based PK, PBPK) approaches were applied to enhance confidence of recommendation and facilitate the clinical development through scenario simulations. The PopPK model identified food (for absorption rate constant (Ka)) and proton pump inhibitors (PPI, for relative bioavailability (Frel) and Ka) as significant covariates. Food and PPI also impacted the variability of Frel. The PBPK model accounted for the supersaturation tendency of pictilisib, and gastric emptying physiology successfully predicted the food and PPI effect on pictilisib absorption. Our research highlights the importance of applying both quantitative approaches to address critical drug development questions.
机译:Pictilisib是一种弱碱性化合物,是口服的,有效的和选择性的泛磷脂酰肌醇3激酶泛抑制剂,可用于肿瘤适应症。为了研究高脂食物和胃酸pH值对Pictilisib药代动力学(PK)的重要性并提出标签建议,对健康志愿者进行了专门的临床研究,从上至下(人口PK,PopPK)和自下而上(生理上)应用基于PK,PBPK的方法来增强推荐的置信度,并通过情景模拟促进临床发展。 PopPK模型将食物(对于吸收速率常数(Ka))和质子泵抑制剂(PPI,对于相对生物利用度(Frel)和Ka)确定为重要的协变量。食物和PPI也影响Frel的可变性。 PBPK模型解释了Pictilisib的过饱和趋势,并且胃排空生理学成功地预测了食物和PPI对Pictilisib吸收的影响。我们的研究突出了应用两种定量方法来解决关键药物开发问题的重要性。

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