依度沙班在日本成年房颤患者中的群体药代动力学和药物基因组学
Population pharmacokinetics and pharmacogenomics of edoxaban in Japanese adults with atrial fibrillation.
作者信息
Ueshima Satoshi, Hira Daiki, Matsuda Sayana, Michihata Rio, Tabuchi Yohei, Ozawa Tomoya, Itoh Hideki, Iguchi Moritake, Akao Masaharu, Aizawa Takanori, Kashiwa Asami, Shizuta Satoshi, Makiyama Takeru, Nakagawa Yoshihisa, Horie Minoru, Terada Tomohiro, Katsura Toshiya
机构信息
College of Pharmaceutical Sciences, Ritsumeikan University, 1-1-1 Noji- higashi, Kusatsu, Shiga, 525-8577, Japan.
Department of Pharmacy, Shiga University of Medical Science Hospital, Seta Tsukinowa-Cho, Otsu, Shiga, 520-2192, Japan.
出版信息
J Pharm Health Care Sci. 2025 Jun 2;11(1):46. doi: 10.1186/s40780-025-00453-2.
BACKGROUND
Edoxaban is used as an anti-coagulant to prevent cardioembolic infarction, deep vein thrombosis, and pulmonary embolism. Edoxaban pharmacokinetics have been reported to be affected by several factors such as renal function, age, body weight, and the concomitant use of P-glycoprotein inhibitors. However, the relationship between genetic polymorphisms in drug metabolizing enzymes and transporters and the inter-individual variability of edoxaban pharmacokinetics in patients with atrial fibrillation (AF) remains unclear. Additionally, there is little information concerning PPK analysis using real world data. In this study a population pharmacokinetic and pharmacogenomic analysis was conducted to clarify covariate factors affecting the edoxaban pharmacokinetics in Japanese adult AF patients.
METHODS
One hundred and thirty-one blood samples were collected from 131 patients. The edoxaban pharmacokinetic profile was described by a one-compartment model, and pharmacogenomic data were stratified according to CYP3A5 (CYP3A5*3) and ABCB1 (ABCB1 1236 C > T, 2677G > T/A, and 3435 C > T) polymorphisms. A non-linear mixed-effects modeling software (NONMEM™) was used to evaluate the effects of patient characteristics and genetic polymorphisms on the edoxaban pharmacokinetics.
RESULTS
The apparent oral clearance (CL/F) of edoxaban was estimated, and the apparent volume of distribution was fixed at the reported value. The CL/F of edoxaban was correlated non-linearly with creatinine clearance (CLcr), wherein the population mean CL/F for a typical patient (CLcr = 61.8 mL/min) was estimated to be 28.2 L/h. Other clinical laboratory data and genetic polymorphisms, excluding CLcr, did not affect the edoxaban pharmacokinetics.
CONCLUSIONS
These results suggest that genetic polymorphisms of CYP3A5 and ABCB1 are not considered intrinsic factors affecting edoxaban pharmacokinetics in Japanese adult AF patients. Similarly to previous studies, renal function affects its pharmacokinetics. These findings may provide useful information for individualized anticoagulant therapy with edoxaban to prevent adverse events without reference to genetic polymorphisms of CYP3A5 and ABCB1.
背景
依度沙班用作抗凝剂,以预防心源性栓塞性梗死、深静脉血栓形成和肺栓塞。据报道,依度沙班的药代动力学受多种因素影响,如肾功能、年龄、体重以及P-糖蛋白抑制剂的联合使用。然而,药物代谢酶和转运体的基因多态性与心房颤动(AF)患者依度沙班药代动力学的个体间变异性之间的关系仍不清楚。此外,关于使用真实世界数据进行群体药代动力学(PPK)分析的信息很少。在本研究中,进行了群体药代动力学和药物基因组学分析,以阐明影响日本成年AF患者依度沙班药代动力学的协变量因素。
方法
从131例患者中采集了131份血样。依度沙班的药代动力学特征用单室模型描述,药物基因组学数据根据CYP3A5(CYP3A5*3)和ABCB1(ABCB1 1236 C>T、2677G>T/A和3435 C>T)多态性进行分层。使用非线性混合效应建模软件(NONMEM™)评估患者特征和基因多态性对依度沙班药代动力学的影响。
结果
估算了依度沙班的表观口服清除率(CL/F),并将分布容积固定为报道值。依度沙班的CL/F与肌酐清除率(CLcr)呈非线性相关,其中典型患者(CLcr = 61.8 mL/min)的群体平均CL/F估计为28.2 L/h。除CLcr外,其他临床实验室数据和基因多态性均不影响依度沙班的药代动力学。
结论
这些结果表明,CYP3A5和ABCB1的基因多态性并非影响日本成年AF患者依度沙班药代动力学的内在因素。与先前的研究相似,肾功能会影响其药代动力学。这些发现可能为依度沙班个体化抗凝治疗提供有用信息,以预防不良事件,而无需考虑CYP3A5和ABCB1的基因多态性。
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