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Pharmacokinetic profile of the oral direct thrombin inhibitor dabigatran etexilate in healthy volunteers and patients undergoing total hip replacement.口服直接凝血酶抑制剂达比加群酯在健康志愿者和接受全髋关节置换术患者中的药代动力学特征。
J Clin Pharmacol. 2005 May;45(5):555-63. doi: 10.1177/0091270005274550.
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A new oral direct thrombin inhibitor, dabigatran etexilate, compared with enoxaparin for prevention of thromboembolic events following total hip or knee replacement: the BISTRO II randomized trial.一种新型口服直接凝血酶抑制剂达比加群酯与依诺肝素相比用于预防全髋关节或全膝关节置换术后血栓栓塞事件:BISTRO II随机试验
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新型口服直接凝血酶抑制剂达比加群酯在健康男性受试者中的药代动力学、药效学及耐受性

The pharmacokinetics, pharmacodynamics and tolerability of dabigatran etexilate, a new oral direct thrombin inhibitor, in healthy male subjects.

作者信息

Stangier Joachim, Rathgen Karin, Stähle Hildegard, Gansser Dietmar, Roth Willy

机构信息

Boehringer Ingelheim Pharma GmbH & Co KG, Ingelheim, Germany.

出版信息

Br J Clin Pharmacol. 2007 Sep;64(3):292-303. doi: 10.1111/j.1365-2125.2007.02899.x. Epub 2007 May 15.

DOI:10.1111/j.1365-2125.2007.02899.x
PMID:17506785
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2000643/
Abstract

AIMS

The novel direct thrombin inhibitor (DTI), dabigatran etexilate (Boehringer Ingelheim Pharma GmbH & Co. KG), shows potential as an oral antithrombotic agent. Two double-blind, randomized trials were undertaken to investigate the pharmacokinetics (PK), pharmacodynamics (PD) and tolerability of orally administered dabigatran etexilate in healthy male subjects.

METHODS

Dabigatran etexilate or placebo was administered orally at single doses of 10-400 mg (n = 40) or at multiple doses of 50-400 mg three times daily for 6 days (n = 40). Plasma and urine samples were collected over time to determine the PK profile of dabigatran. PD activity was assessed by its effects on blood coagulation parameters: activated partial thromboplastin time (aPTT), prothrombin time (PT), reported as international normalized ratio (INR), thrombin time (TT), and ecarin clotting time (ECT). All adverse events were recorded.

RESULTS

Dabigatran etexilate was rapidly absorbed with peak plasma concentrations of dabigatran reached within 2 h of administration. This was followed by a rapid distribution/elimination phase and a terminal phase, with associated estimated half-lives of 8-10 h and 14-17 h with single and multiple dose administrations, respectively. Dabigatran exhibited linear PK characteristics with dose-proportional increases observed in maximum plasma concentration and area under the curve. Steady-state conditions were reached within 3 days with multiple dosing. The mean apparent volume of distribution during the terminal phase (V(z)/F) of 1860 l (range 1430-2400 l) and the apparent total clearance after oral administration (CL(tot)/F) of 2031 ml min(-1) (range 1480-2430), were dose independent. Time curves for aPTT, INR, TT and ECT paralleled plasma concentration-time curves with values increasing rapidly and in a dose-dependent manner. At the highest dose of 400 mg administered three times daily, maximum prolongations over baseline of 3.1 (aPTT), 3.5 (INR), 29 (TT) and 9.5-fold (ECT) were observed. Dabigatran underwent conjugation with glucuronic acid to form pharmacologically active conjugates that accounted for approximately 20% of total dabigatran in plasma. Overall, variability in PK parameters was low to moderate, with an average interindividual coefficient of variation (CV) of approximately 30% and variability in PD parameters was low, with CV < 10%. Of the four assays, TT and ECT exhibited the greatest sensitivity and precision within the anticipated therapeutic dose range. Bleeding events were few and were mild-to-moderate in intensity, occurring only in the higher, multiple dose groups.

CONCLUSIONS

These data suggest that dabigatran etexilate is a promising novel oral DTI with predictable PK and PD characteristics and good tolerability. Further investigation of dabigatran etexilate for the treatment and prophylaxis of patients with arterial and venous thromboembolic disorders, acute coronary syndromes and other medical conditions is warranted.

摘要

目的

新型直接凝血酶抑制剂(DTI)达比加群酯(勃林格殷格翰制药有限公司)显示出作为口服抗血栓药物的潜力。进行了两项双盲随机试验,以研究健康男性受试者口服达比加群酯的药代动力学(PK)、药效动力学(PD)和耐受性。

方法

达比加群酯或安慰剂以10 - 400 mg的单剂量(n = 40)或50 - 400 mg的多剂量每日三次给药,共6天(n = 40)。随时间收集血浆和尿液样本,以确定达比加群的PK曲线。通过其对凝血参数的影响评估PD活性:活化部分凝血活酶时间(aPTT)、凝血酶原时间(PT),以国际标准化比值(INR)报告、凝血酶时间(TT)和蛇静脉酶凝血时间(ECT)。记录所有不良事件。

结果

达比加群酯吸收迅速,给药后2小时内达比加群血浆浓度达到峰值。随后是快速分布/消除期和终末期,单次和多次给药的相关估计半衰期分别为8 - 10小时和14 - 17小时。达比加群表现出线性PK特征,最大血浆浓度和曲线下面积随剂量成比例增加。多次给药3天内达到稳态。终末期平均表观分布容积(V(z)/F)为1860升(范围1430 - 2400升),口服给药后表观总清除率(CL(tot)/F)为2031毫升/分钟(范围1480 - 2430),与剂量无关。aPTT、INR、TT和ECT的时间曲线与血浆浓度 - 时间曲线平行,值迅速增加且呈剂量依赖性。每日三次给药最高剂量400 mg时,观察到aPTT、INR、TT和ECT相对于基线的最大延长倍数分别为3.1倍、3.5倍、29倍和9.5倍。达比加群与葡萄糖醛酸结合形成药理活性共轭物,约占血浆中达比加群总量的20%。总体而言,PK参数的变异性低至中等,个体间平均变异系数(CV)约为30%,PD参数的变异性低,CV < 10%。在四种检测方法中,TT和ECT在预期治疗剂量范围内表现出最大的敏感性和精密度。出血事件较少,强度为轻度至中度,仅发生在较高剂量的多剂量组中。

结论

这些数据表明达比加群酯是一种有前景的新型口服DTI,具有可预测的PK和PD特征以及良好的耐受性。有必要进一步研究达比加群酯用于治疗和预防动脉和静脉血栓栓塞性疾病、急性冠状动脉综合征及其他病症的患者。