Wåhlander Karin, Eriksson-Lepkowska Maria, Frison Lars, Fager Gunnar, Eriksson Ulf G
Experimental Medicine, AstraZeneca R&D, Mölndal, Sweden.
Clin Pharmacokinet. 2003;42(8):755-64. doi: 10.2165/00003088-200342080-00004.
The oral direct thrombin inhibitor ximelagatran is a new class of anticoagulant currently in clinical development for the prevention and treatment of thromboembolic disease. After oral administration, ximelagatran is rapidly absorbed and bioconverted to its active form melagatran.
To investigate the influence of mild-to-moderate hepatic impairment on the pharmacokinetic and pharmacodynamic properties of ximelagatran.
Nonblinded, nonrandomised study.
Twelve volunteers with mild-to-moderate hepatic impairment (classified as Child-Pugh A or B) and 12 age-, weight-, and sex-matched control volunteers with normal hepatic function.
Volunteers received a single oral dose of ximelagatran 24mg. Plasma and urine samples were collected for pharmacokinetic and pharmacodynamic analyses.
The absorption and bioconversion of ximelagatran to melagatran were rapid in both groups. The maximum plasma concentration of melagatran (Cmax) was achieved 2-3 hours after administration; the mean elimination half-life (t1/2z) was 3.6 hours for hepatically impaired volunteers and 3.1 hours for the control volunteers. The area under the plasma concentration-time curve (AUC) and Cmax of melagatran in volunteers with hepatic impairment were 11 and 25% lower than in control volunteers, respectively. However, after correcting for the higher renal function (i.e. higher calculated creatinine clearance) in the hepatically impaired volunteers, the ratio of melagatran AUC for hepatically impaired/control volunteers was 0.98 (90% CI 0.80, 1.22), suggesting that mild-to-moderate hepatic impairment had no influence on the pharmacokinetics of ximelagatran. Melagatran was the predominant compound in urine, accounting for 13-14% of the ximelagatran dose. Renal clearance of melagatran was 13% higher in hepatically impaired than in control volunteers. There were no significant differences between the two groups in the concentration-response relationship between plasma melagatran concentration and activated partial thromboplastin time (APTT). Baseline prothrombin time (PT) was slightly longer in the hepatically impaired patients than in the control volunteers, probably reflecting a slight decrease in the activity of coagulation factors. However, when concentrations of melagatran were at their peak, the increase in PT from baseline values was the same in both groups. Capillary bleeding time was measured in the hepatically impaired patients only, and was not increased by ximelagatran. Ximelagatran was well tolerated in both groups.
There were no differences in the pharmacokinetic or pharmacodynamic properties of melagatran following oral administration of ximelagatran between the hepatically impaired and control volunteers. These findings suggest that dose adjustment for patients with mild-to-moderate impairment of hepatic function is not necessary.
口服直接凝血酶抑制剂希美加群是一类新型抗凝剂,目前正处于预防和治疗血栓栓塞性疾病的临床开发阶段。口服后,希美加群迅速吸收并生物转化为其活性形式美拉加群。
研究轻度至中度肝功能损害对希美加群药代动力学和药效学特性的影响。
非盲、非随机研究。
12名轻度至中度肝功能损害的志愿者(Child-Pugh A或B级)和12名年龄、体重和性别匹配的肝功能正常的对照志愿者。
志愿者单次口服24mg希美加群。采集血浆和尿液样本进行药代动力学和药效学分析。
两组中希美加群向美拉加群的吸收和生物转化均迅速。给药后2 - 3小时达到美拉加群的最大血浆浓度(Cmax);肝功能受损志愿者的平均消除半衰期(t1/2z)为3.6小时,对照志愿者为3.1小时。肝功能受损志愿者中美拉加群的血浆浓度-时间曲线下面积(AUC)和Cmax分别比对照志愿者低11%和25%。然而,校正肝功能受损志愿者较高的肾功能(即较高的计算肌酐清除率)后,肝功能受损/对照志愿者的美拉加群AUC比值为0.98(90%CI 0.80,1.22),表明轻度至中度肝功能损害对希美加群的药代动力学无影响。美拉加群是尿液中的主要化合物,占希美加群剂量的13 - 14%。肝功能受损志愿者中美拉加群的肾清除率比对照志愿者高13%。两组间血浆美拉加群浓度与活化部分凝血活酶时间(APTT)之间的浓度-反应关系无显著差异。肝功能受损患者的基线凝血酶原时间(PT)略长于对照志愿者,这可能反映了凝血因子活性略有降低。然而,当美拉加群浓度达到峰值时,两组中PT相对于基线值的增加相同。仅在肝功能受损患者中测量了毛细血管出血时间,希美加群未使其增加。两组对希美加群的耐受性均良好。
肝功能受损和对照志愿者口服希美加群后,美拉加群的药代动力学和药效学特性无差异。这些发现表明,轻度至中度肝功能损害患者无需调整剂量。
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