Evaluation of pharmacokinetics of warfarin from validated pharmacokinetic-pharmacodynamic model

IF 3.4 Q2 CHEMISTRY, MEDICINAL
ADMET and DMPK Pub Date : 2021-01-18 DOI:10.5599/admet.909
K. Sridharan, R. Al Banna, Aysha A Husain
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引用次数: 0

Abstract

Background Pharmacokinetics of warfarin has not been described in our population. We derived the pharmacokinetic parameters from a validated pharmacokinetic-pharmacodynamic model. Methods Patients receiving warfarin for at least 6 months were recruited and their demographic characteristics, prothrombin time international normalized ratio (PT-INR), warfarin doses and concomitant drugs were collected. Using a validated pharmacokinetic-pharmacodynamic model, we predicted maximum plasma concentration (Cmax), total clearance (CL), volume of distribution (Vd) and elimination rate (k). Warfarin sensitive index (WSI) and warfarin composite measures (WCM) were estimated from the dose and INR values. Liver weight was predicted using validated formula. Results Two-hundred and twenty patients were recruited. The following were the predicted pharmacokinetic parameters: Cmax (mg/L) was 5.8 (0.4); k (L/day) was 1 (0.1); CL (L/day) was 2.1 (0.2); and Vd (L) was 7.6 (0.2). Patients with Cmax and elimination rate outside the mean+1.96 SD had significantly lower WSI and higher WCM. Significant correlations were observed between Cmax with CL, Vd, and k of warfarin. Significant correlations were also observed between CL and Vd of warfarin with liver weight of the study participants. Conclusion We predicted pharmacokinetic parameters of warfarin from the validated pharmacokinetic-pharmacodynamic model in our population. More studies are needed exploring the relationship between various pharmacodynamic indices of warfarin and pharmacokinetic parameters of warfarin.
从有效的药动学-药效学模型评价华法林的药动学
背景:华法林的药代动力学在我国人群中尚未被描述。我们从经过验证的药代动力学-药效学模型中推导出药代动力学参数。方法收集接受华法林治疗6个月以上患者的人口学特征、凝血酶原时间国际标准化比值(PT-INR)、华法林剂量及伴随用药情况。通过验证的药代动力学-药效学模型,我们预测了最大血浆浓度(Cmax)、总清除率(CL)、分布体积(Vd)和清除率(k),并根据剂量和INR值估计了华法林敏感指数(WSI)和华法林复合测量值(WCM)。采用验证公式预测肝脏重量。结果共纳入220例患者。预测药代动力学参数为:Cmax (mg/L)为5.8 (0.4);k (L/day) = 1 (0.1);CL (L/day)为2.1 (0.2);Vd (L)为7.6(0.2)。Cmax和清除率在平均值+1.96 SD之外的患者WSI显著降低,WCM显著升高。Cmax与华法林的CL、Vd、k呈显著相关。华法林的CL和Vd与研究参与者的肝脏重量也有显著的相关性。结论我们通过验证的华法林药动学-药效学模型预测了华法林在我国人群中的药动学参数。华法林的各种药效学指标与药动学参数之间的关系有待进一步研究。
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来源期刊
ADMET and DMPK
ADMET and DMPK Multiple-
CiteScore
4.40
自引率
0.00%
发文量
22
审稿时长
4 weeks
期刊介绍: ADMET and DMPK is an open access journal devoted to the rapid dissemination of new and original scientific results in all areas of absorption, distribution, metabolism, excretion, toxicology and pharmacokinetics of drugs. ADMET and DMPK publishes the following types of contributions: - Original research papers - Feature articles - Review articles - Short communications and Notes - Letters to Editors - Book reviews The scope of the Journal involves, but is not limited to, the following areas: - physico-chemical properties of drugs and methods of their determination - drug permeabilities - drug absorption - drug-drug, drug-protein, drug-membrane and drug-DNA interactions - chemical stability and degradations of drugs - instrumental methods in ADMET - drug metablic processes - routes of administration and excretion of drug - pharmacokinetic/pharmacodynamic study - quantitative structure activity/property relationship - ADME/PK modelling - Toxicology screening - Transporter identification and study
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