An open-label study to explore the optimal design of CYP3A drug-drug interaction clinical trials in healthy Chinese people.

IF 2.9 4区 医学 Q2 PHARMACOLOGY & PHARMACY Pharmacology Research & Perspectives Pub Date : 2024-08-01 DOI:10.1002/prp2.1252
Jingcheng Chen, Jiangshuo Li, Jingxuan Wu, Yuqin Song, Lijun Li, Jianxiong Zhang, Ruihua Dong
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Abstract

A drug-drug interaction (DDI) trial of cytochrome P450 3A (CYP3A) is a necessary part of early-phase trials of drugs mainly metabolized by this enzyme, but CYP3A DDI clinical trials do not have a standard design, especially for Chinese people. We aimed to offer specific recommendations for CYP3A DDI clinical trial design. This was an open, three-cycle, self-controlled study. Healthy subjects were given different administration strategies of CYP3A4 perpetrators. In each cycle, blood samples were collected before and within 24 h after the administration of midazolam, the CYP3A indicator substrate. The plasma concentrations of midazolam and 1-hydroxymidazolam was obtained using liquid chromatography tandem mass spectrometry assay. For CYP3A inhibition, itraconazole exposure with a loading dose could increase the exposure of midazolam by 3.21-fold based on maximum plasma concentration (Cmax), 8.37-fold based on area under the curve Pharmacology Research & Perspectives for review only from zero to the time point (AUC0-t), and 11.22-fold based on area under the curve from zero to infinity (AUC0-∞). The data were similar for itraconazole pretreatment without a loading dose. For CYP3A induction, the exposure of rifampin for 7 days decreased the plasma concentration of midazolam ~0.27-fold based on Cmax, ~0.18-fold based on AUC0-t, and ~0.18-fold based on AUC0-∞. Midazolam exposure did not significantly change when the pretreatment of rifampin increased to 14 days. This study showed that itraconazole pretreatment for 3 days without a loading dose was enough for CYP3A inhibition, and pretreatment with rifampin for 7 days could induce near-maximal CYP3A levels.

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一项开放标签研究,探索在健康中国人中进行 CYP3A 药物相互作用临床试验的最佳设计。
细胞色素P450 3A(CYP3A)药物相互作用(DDI)试验是主要由该酶代谢的药物早期试验的必要组成部分,但CYP3A DDI临床试验并没有标准的设计,尤其是针对中国人。我们旨在为 CYP3A DDI 临床试验设计提供具体建议。这是一项开放式、三周期、自控研究。给健康受试者使用不同的 CYP3A4 致效剂给药策略。在每个周期中,在服用 CYP3A 指示底物咪达唑仑之前和之后 24 小时内采集血样。使用液相色谱串联质谱法测定咪达唑仑和 1-hydroxymidazolam 的血浆浓度。在 CYP3A 抑制方面,根据最大血浆浓度(Cmax)计算,伊曲康唑的负荷剂量可使咪达唑仑的暴露量增加 3.21 倍;根据从零到时间点的曲线下面积(AUC0-t)计算,可使咪达唑仑的暴露量增加 8.37 倍;根据从零到无穷大的曲线下面积(AUC0-∞)计算,可使咪达唑仑的暴露量增加 11.22 倍。伊曲康唑预处理无负荷剂量时的数据类似。就 CYP3A 诱导而言,利福平暴露 7 天后,咪达唑仑的血浆浓度按 Cmax 计算下降了 ~0.27 倍,按 AUC0-t 计算下降了 ~0.18 倍,按 AUC0-∞ 计算下降了 ~0.18 倍。当利福平的预处理时间增加到 14 天时,咪达唑仑的暴露量没有明显变化。本研究表明,伊曲康唑预处理 3 天且不加负荷剂量足以抑制 CYP3A,而利福平预处理 7 天可诱导接近最大的 CYP3A 水平。
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来源期刊
Pharmacology Research & Perspectives
Pharmacology Research & Perspectives Pharmacology, Toxicology and Pharmaceutics-General Pharmacology, Toxicology and Pharmaceutics
CiteScore
5.30
自引率
3.80%
发文量
120
审稿时长
20 weeks
期刊介绍: PR&P is jointly published by the American Society for Pharmacology and Experimental Therapeutics (ASPET), the British Pharmacological Society (BPS), and Wiley. PR&P is a bi-monthly open access journal that publishes a range of article types, including: target validation (preclinical papers that show a hypothesis is incorrect or papers on drugs that have failed in early clinical development); drug discovery reviews (strategy, hypotheses, and data resulting in a successful therapeutic drug); frontiers in translational medicine (drug and target validation for an unmet therapeutic need); pharmacological hypotheses (reviews that are oriented to inform a novel hypothesis); and replication studies (work that refutes key findings [failed replication] and work that validates key findings). PR&P publishes papers submitted directly to the journal and those referred from the journals of ASPET and the BPS
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