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具有非典型分布行为药物的生理药代动力学模型的开发与验证:地昔帕明案例研究

Development and Qualification of Physiologically Based Pharmacokinetic Models for Drugs With Atypical Distribution Behavior: A Desipramine Case Study.

作者信息

Samant T S, Lukacova V, Schmidt S

机构信息

Center for Pharmacometrics and Systems Pharmacology, Department of Pharmaceutics, College of Pharmacy, University of Florida, Lake Nona (Orlando), Florida, USA.

Simulations Plus, Inc., Lancaster, California, USA.

出版信息

CPT Pharmacometrics Syst Pharmacol. 2017 May;6(5):315-321. doi: 10.1002/psp4.12180. Epub 2017 Apr 11.

Abstract

Desipramine is a secondary tricyclic amine, which is primarily metabolized by cytochrome 2D6. It shows a high volume of distribution (Vss) (10-50 L/kg) due to its high lipophilicity, unspecific phospholipid binding, and lysosomal trapping. The objective of this study was to develop and qualify a physiologically based pharmacokinetic (PBPK) model for desipramine, which accounts for the high Vss of the drug following intravenous and oral administration of doses up to 100 mg. The model also accounts for the extended time to reach maximum concentration after oral dosing due to enterocyte trapping. Once developed and qualified in adults, we characterized the dynamic changes in metabolism and pharmacokinetics of desipramine after birth by scaling the system-specific parameters of the model from adults to pediatrics. The developed modeling strategy provides a prototypical workflow that can also be applied to other drugs with similar properties and a high volume of distribution.

摘要

地昔帕明是一种二级三环胺,主要通过细胞色素2D6代谢。由于其高亲脂性、非特异性磷脂结合和溶酶体捕获作用,它表现出高分布容积(Vss)(10 - 50 L/kg)。本研究的目的是开发并验证一种基于生理的地昔帕明药代动力学(PBPK)模型,该模型可解释静脉注射和口服高达100 mg剂量后该药物的高Vss。该模型还考虑了由于肠细胞捕获导致口服给药后达到最大浓度的时间延长。在成人体内开发并验证该模型后,我们通过将模型的系统特异性参数从成人按比例缩放至儿科,来表征地昔帕明出生后代谢和药代动力学的动态变化。所开发的建模策略提供了一种原型工作流程,该流程也可应用于其他具有相似性质和高分布容积的药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b549/5697013/ef39eebb9bf9/PSP4-6-315-g001.jpg

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