Pharmacokinetic and Pharmacodynamic Interaction of Finerenone with Diltiazem, Fluconazole, and Ritonavir in Rats.

IF 1.9 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Tham Thi Bui, So-Hyeon Kim, Woojin Jung, Sung-Yoon Yang, Quyen Thi Tran, Hyunjung Lee, Seongwon Park, Lien Thi Ngo, Hwi-Yeol Yun, Jung-Woo Chae
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引用次数: 0

Abstract

Background and objectives: Finerenone, a novel selective non-steroidal mineralocorticoid receptor antagonist, has been indicated in chronic kidney disease associated with type 2 diabetes mellitus. Considering the potential complications of diabetes, finerenone can be co-administered with various drugs, including fluconazole, diltiazem, and ritonavir. Given that finerenone is a substrate of cytochrome P450 (CYP) 3A4, the concurrent administration of finerenone with CYP3A4 inhibitors (diltiazem or fluconazole or ritonavir) could potentially lead to drug interactions, which may cause adverse events such as hyperkalemia. No studies have investigated interactions between finerenone and diltiazem or fluconazole or ritonavir. Therefore, this study aims to investigate the pharmacokinetic interaction of finerenone with diltiazem or fluconazole or ritonavir and to evaluate the impact of fluconazole on the pharmacodynamics of finerenone.

Methods: The pharmacokinetic study included four rat groups (n = 8 rats/group), including a control group (finerenone alone) and test groups (finerenone pretreated with diltiazem or fluconazole or ritonavir) using both non-compartment analysis (NCA) and population pharmacokinetic (pop-PK) modeling. The pop-PK model was developed using non-linear mixed-effects modeling in NONMEM® (version 7.5.0). In the pharmacodynamic study, serum potassium (K+) levels were measured to assess the effects of fluconazole on finerenone-induced hyperkalemia.

Results: The NCA results indicated that the area under the plasma concentration-time curve (AUC) of finerenone increased by 1.86- and 1.95-fold when coadministered with fluconazole and ritonavir, respectively. In contrast, diltiazem did not affect the pharmacokinetics of finerenone. The pharmacokinetic profiles of finerenone were best described by a one-compartment disposition with first-order elimination and dual first-order absorption kinetics. The pop-PK modeling results demonstrated that the apparent clearance of finerenone decreased by 50.3% and 49.2% owing to the effects of fluconazole and ritonavir, respectively. Additionally, the slow absorption rate, which represents the absorption in the distal intestinal tract of finerenone, increased by 55.7% due to the effect of ritonavir. Simultaneously, a pharmacodynamic study revealed that finerenone in the presence of fluconazole caused a significant increase in K+ levels compared with finerenone alone.

Conclusions: Coadministration of finerenone with fluconazole or ritonavir increased finerenone exposure in rats. Additionally, the administration of finerenone in the presence of fluconazole resulted in elevated K+ levels in rats. Further clinical studies are required to validate these findings.

大鼠体内非格列酮与地尔硫卓、氟康唑和利托那韦的药代动力学和药效学相互作用
背景和目的:非格列酮(一种新型选择性非甾体类矿物皮质激素受体拮抗剂)已被用于治疗与 2 型糖尿病相关的慢性肾病。考虑到糖尿病的潜在并发症,非格列酮可与多种药物合用,包括氟康唑、地尔硫卓和利托那韦。鉴于非格列酮是细胞色素 P450 (CYP) 3A4 的底物,因此非格列酮与 CYP3A4 抑制剂(地尔硫卓或氟康唑或利托那韦)同时服用可能会导致药物相互作用,从而引发高钾血症等不良事件。目前还没有研究调查非格列酮与地尔硫卓或氟康唑或利托那韦之间的相互作用。因此,本研究旨在探讨非格列酮与地尔硫卓或氟康唑或利托那韦的药代动力学相互作用,并评估氟康唑对非格列酮药效学的影响:药代动力学研究包括四组大鼠(n = 8只/组),包括对照组(单独使用非格列酮)和试验组(使用地尔硫卓或氟康唑或利托那韦预处理非格列酮),采用非室分析(NCA)和群体药代动力学(pop-PK)模型。pop-PK模型是在NONMEM®(7.5.0版)中使用非线性混合效应模型建立的。在药效学研究中,测定了血清钾(K+)水平,以评估氟康唑对非利眠宁诱导的高钾血症的影响:NCA结果表明,与氟康唑和利托那韦合用时,非格列酮的血浆浓度-时间曲线下面积(AUC)分别增加了1.86倍和1.95倍。相比之下,地尔硫卓不会影响非格列酮的药代动力学。非格列酮的药代动力学特征最好用一室处置、一阶消除和双一阶吸收动力学来描述。pop-PK 模型结果表明,由于氟康唑和利托那韦的影响,非格列酮的表观清除率分别降低了 50.3% 和 49.2%。此外,由于利托那韦的作用,代表非格列酮在远端肠道吸收的缓慢吸收率增加了 55.7%。同时,一项药效学研究显示,与单独服用非奈酮相比,非奈酮在氟康唑存在的情况下会导致K+水平显著升高:结论:非格列酮与氟康唑或利托那韦同时给药会增加大鼠的非格列酮暴露量。此外,在氟康唑存在的情况下服用非格列酮会导致大鼠体内 K+ 水平升高。需要进一步的临床研究来验证这些发现。
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
CiteScore
3.70
自引率
0.00%
发文量
64
审稿时长
>12 weeks
期刊介绍: Hepatology International is a peer-reviewed journal featuring articles written by clinicians, clinical researchers and basic scientists is dedicated to research and patient care issues in hepatology. This journal focuses mainly on new and emerging diagnostic and treatment options, protocols and molecular and cellular basis of disease pathogenesis, new technologies, in liver and biliary sciences. Hepatology International publishes original research articles related to clinical care and basic research; review articles; consensus guidelines for diagnosis and treatment; invited editorials, and controversies in contemporary issues. The journal does not publish case reports.
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