从危害到风险优先排序:利用生理学动力学模型预测药物诱发胆汁淤积的案例研究。

IF 4.8 2区 医学 Q1 TOXICOLOGY
Véronique M. P. de Bruijn, Ivonne M. C. M. Rietjens
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引用次数: 0

摘要

胆汁淤积症的特点是胆汁酸在肝脏积聚。胆汁淤积症的临床表现仅发生在一小部分暴露个体中。本研究旨在开发一种新的方法(NAM),用于预测药物诱导的胆汁淤积症,胆汁淤积症是药物诱导的肝胆汁酸外排抑制和由此导致的胆汁酸蓄积的结果。为此,我们利用通用的生理学动力学(PBK)药物模型预测了一系列药物的肝脏浓度。这些药物对肝脏胆汁酸外流的影响被纳入胆汁酸的 PBK 模型。预测的胆汁酸累积量被用来衡量药物的利胆作用。所选药物在原代悬浮培养肝细胞试验中可抑制肝脏胆汁酸外流,并根据胆汁淤积发生率分为常见、罕见或无。常见胆汁淤积药物包括阿托伐他汀、氯丙嗪、环孢素、格列美脲、酮康唑和利托那韦。这些药物的胆汁淤积发生率似乎不能根据其抑制肝脏胆汁酸外流的 Ki 值来充分预测,而是根据 PBK 模型预测的肝脏内部药物浓度在治疗剂量水平高于 Ki 值时的 AUC 值来预测。如果药物清除速度较慢、胆汁酸池较大、胆盐输出泵(BSEP)丰度降低或给药剂量高于治疗剂量水平,则预测发生药物性胆汁淤积的风险较高。这些结果提供了一个使用基于 PBK 的 NAM 进行胆汁淤积风险优先排序的原则性证明,该 NAM 是转运体抑制和个体风险因素识别的结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

From hazard to risk prioritization: a case study to predict drug-induced cholestasis using physiologically based kinetic modeling

From hazard to risk prioritization: a case study to predict drug-induced cholestasis using physiologically based kinetic modeling

Cholestasis is characterized by hepatic accumulation of bile acids. Clinical manifestation of cholestasis only occurs in a small proportion of exposed individuals. The present study aims to develop a new approach methodology (NAM) to predict drug-induced cholestasis as a result of drug-induced hepatic bile acid efflux inhibition and the resulting bile acid accumulation. To this end, hepatic concentrations of a panel of drugs were predicted by a generic physiologically based kinetic (PBK) drug model. Their effects on hepatic bile acid efflux were incorporated in a PBK model for bile acids. The predicted bile acid accumulation was used as a measure for a drug’s cholestatic potency. The selected drugs were known to inhibit hepatic bile acid efflux in an assay with primary suspension-cultured hepatocytes and classified as common, rare, or no for cholestasis incidence. Common cholestasis drugs included were atorvastatin, chlorpromazine, cyclosporine, glimepiride, ketoconazole, and ritonavir. The cholestasis incidence of the drugs appeared not to be adequately predicted by their Ki for inhibition of hepatic bile acid efflux, but rather by the AUC of the PBK model predicted internal hepatic drug concentration at therapeutic dose level above this Ki. People with slower drug clearance, a larger bile acid pool, reduced bile salt export pump (BSEP) abundance, or given higher than therapeutic dose levels were predicted to be at higher risk to develop drug-induced cholestasis. The results provide a proof-of-principle of using a PBK-based NAM for cholestasis risk prioritization as a result of transporter inhibition and identification of individual risk factors.

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来源期刊
Archives of Toxicology
Archives of Toxicology 医学-毒理学
CiteScore
11.60
自引率
4.90%
发文量
218
审稿时长
1.5 months
期刊介绍: Archives of Toxicology provides up-to-date information on the latest advances in toxicology. The journal places particular emphasis on studies relating to defined effects of chemicals and mechanisms of toxicity, including toxic activities at the molecular level, in humans and experimental animals. Coverage includes new insights into analysis and toxicokinetics and into forensic toxicology. Review articles of general interest to toxicologists are an additional important feature of the journal.
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