Coproporphyrin-I as a Selective OATP1B Biomarker Can Be Used to Delineate the Mechanisms of Complex Drug–Drug Interactions: Cedirogant Case Study

IF 6.3 2区医学 Q1 PHARMACOLOGY & PHARMACY

Clinical Pharmacology & Therapeutics Pub Date : 2024-08-05 DOI:10.1002/cpt.3399

Ryota Kikuchi, Yuli Qian, Mohamed Badawi, John P. Savaryn, Shashikanth Gannu, Ann Eldred, Shuai Hao, Ahmed Hamed Salem, Wei Liu, Cheri E. Klein, Mohamed-Eslam F. Mohamed

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Abstract

Cedirogant is an inverse agonist of retinoic acid-related orphan receptor gamma thymus developed for the treatment of chronic plaque psoriasis. Cedirogant induces cytochrome P450 (CYP) 3A4 while inhibiting P-glycoprotein (P-gp), breast cancer resistance protein (BCRP), organic anion transporting polypeptide (OATP) 1B1, and OATP1B3 in vitro. Static drug–drug interactions (DDIs) predictions suggested possible clinical induction of CYP3A4, and inhibition of P-gp, BCRP, and OATP1B1, leading to challenges in interpreting DDI studies between cedirogant and substrates of CYP3A, P-gp, BCRP, and OATP1B1/3. Here the effects of cedirogant on the pharmacokinetics of two statin drugs were investigated in healthy participants. Coproporphyrin-I (CP-I), a selective endogenous OATP1B biomarker, was used to assess the impact of cedirogant on OATP1B. Cedirogant (375 mg once daily) increased rosuvastatin maximum plasma concentration (C_max) and area under the plasma concentration curve (AUC_tau) by 141% and 55%, respectively when co-administered, whereas atorvastatin C_max increased by 40% with no effect on its AUC_tau compared with administration of rosuvastatin/atorvastatin alone. Cedirogant did not increase CP-I exposures, indicating no clinical OATP1B inhibition. The increased rosuvastatin exposure and minimal change in atorvastatin exposure with co-administration of cedirogant is attributed to BCRP inhibition and interplay between P-gp/BCRP inhibition and CYP3A induction, respectively. Correlation analysis with data from two investigational drugs (glecaprevir and flubentylosin) demonstrated that OATP1B1 R-value of > 1.5 and [C_max,u]/[OATP1B1 IC₅₀] of > 0.1 are associated with > 1.25-fold increase in CP-I C_max ratio. This demonstrates the utility of CP-I in disentangling mechanisms underlying a complex DDI involving multiple transporters and enzymes and proposes refined criteria for static OATP1B inhibition predictions.

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Coproporphyrin-I 作为一种选择性 OATP1B 生物标记物，可用于阐明复杂的药物相互作用机制：Cedirogant 案例研究。

Cedirogant 是维甲酸相关孤儿受体 gamma thymus 的反向激动剂，用于治疗慢性斑块状银屑病。Cedirogant 可诱导细胞色素 P450（CYP）3A4，同时在体外抑制 P-糖蛋白（P-gp）、乳腺癌抗性蛋白（BCRP）、有机阴离子转运多肽（OATP）1B1 和 OATP1B3。静态药物相互作用（DDIs）预测表明，临床上可能会诱导 CYP3A4，并抑制 P-gp、BCRP 和 OATP1B1，这给解释 cedirogant 与 CYP3A、P-gp、BCRP 和 OATP1B1/3 底物之间的 DDI 研究带来了挑战。在此，我们以健康参与者为研究对象，探讨了 cedirogant 对两种他汀类药物药代动力学的影响。Coproporphyrin-I（CP-I）是一种选择性内源性 OATP1B 生物标记物，用于评估 cedirogant 对 OATP1B 的影响。与单独服用罗伐他汀/阿托伐他汀相比，联合服用 Cedirogant（375 毫克，每天一次）可使罗伐他汀的最大血浆浓度（Cmax）和血浆浓度曲线下面积（AUCtau）分别增加 141% 和 55%，而阿托伐他汀的 Cmax 增加 40%，但对其 AUCtau 没有影响。Cedirogant不会增加CP-I的暴露量，这表明它对OATP1B没有临床抑制作用。同时服用西地孕酮会增加罗苏伐他汀的暴露量，而阿托伐他汀的暴露量变化很小，这分别归因于BCRP抑制以及P-gp/BCRP抑制和CYP3A诱导之间的相互作用。与两种在研药物（格列卡韦和氟苯尼考）数据的相关性分析表明，OATP1B1 R 值大于 1.5 和[Cmax,u]/[OATP1B1 IC50] 大于 0.1 与 CP-I Cmax 比值增加大于 1.25 倍相关。这证明了 CP-I 在分解涉及多个转运体和酶的复杂 DDI 潜在机制方面的作用，并提出了静态 OATP1B 抑制预测的改进标准。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical Pharmacology & Therapeutics 医学-药学

CiteScore

12.70

自引率

7.50%

发文量

290

审稿时长

2 months

期刊介绍： Clinical Pharmacology & Therapeutics (CPT) is the authoritative cross-disciplinary journal in experimental and clinical medicine devoted to publishing advances in the nature, action, efficacy, and evaluation of therapeutics. CPT welcomes original Articles in the emerging areas of translational, predictive and personalized medicine; new therapeutic modalities including gene and cell therapies; pharmacogenomics, proteomics and metabolomics; bioinformation and applied systems biology complementing areas of pharmacokinetics and pharmacodynamics, human investigation and clinical trials, pharmacovigilence, pharmacoepidemiology, pharmacometrics, and population pharmacology.