静脉注射氯吡格雷(MDCO - 157)与口服氯吡格雷的比较:随机交叉AMPHORE研究。
Intravenous Clopidogrel (MDCO-157) Compared with Oral Clopidogrel: The Randomized Cross-Over AMPHORE Study.
作者信息
Collet Jean-Philippe, Funck-Brentano Christian, Prats Jayne, Salem Joe-Elie, Hulot Jean-Sébastien, Guilloux Edith, Hu Ming-yi, He Kan, Silvain Johanne, Gallois Vanessa, Brugier Delphine, Anzaha Ghalia, Galier Sophie, Nicolas Nathalie, Montalescot Gilles
机构信息
Institut de Cardiologie, INSERM_UMRS 1166, Pitié-Salpêtrière Hospital (AP-HP), Sorbonne Universités UPMC (Paris 6), Paris, France.
ACTION Study Group, Institut de Cardiologie, Bureau 2-236, Pitié-Salpêtrière University Hospital, 47 Boulevard de l'Hôpital, 75013, Paris, France.
出版信息
Am J Cardiovasc Drugs. 2016 Feb;16(1):43-53. doi: 10.1007/s40256-015-0145-0.
BACKGROUND
The extent of P2Y12 inhibition during coronary intervention is an important determinant of ischemic complications. The currently available oral P2Y12 inhibitors are limited by a relatively slow onset of action and variable on-treatment response.
OBJECTIVE
Our objective was to determine the pharmacodynamic (PD) dose-antiplatelet response relationship and the pharmacokinetics of MDCO-157, an intravenous formulation of clopidogrel complexed with sulphobutylether betacyclodextrin, and to identify the dose level of MDCO-157 that matches the PD effect of oral clopidogrel 300 mg.
METHODOLOGY
A randomized open-label crossover study was performed in 33 healthy adult volunteers to determine the pharmacokinetic (clopidogrel and clopidogrel H4 thiol active metabolite) and the PD (vasodilator-stimulated phosphoprotein [VASP]) effects of MDCO-157 at doses of 75, 150, and 300 mg and of oral clopidogrel 300 mg.
RESULTS
Data are presented as %, mean (standard deviation). The maximum effect of P2Y12 receptor inhibition assessed by flow cytometry using VASP was 70.42 (6.7), 69.45 (7.1), and 65.58 (12.6) for intravenous MDCO-157 at doses of 75, 150, and 300 mg, respectively, compared with 56.6 (17.5) with oral clopidogrel 300 mg administration (p < 0.0001). Intravenous administration of MDCO-157 led to a stepwise increase in plasma exposure of clopidogrel, higher than with administration of an oral dose of 300 mg (p < 0.0001). Plasma exposure of H4-thiol also increased with intravenous dose (3.6 ± 2.6, 6.9 ± 4.6, and 12.4 ± 9.1 h·ng/ml for intravenous 75, 150, and 300 mg, respectively) but was lower than with oral administration of a 300-mg dose (34.0 ± 16.0 h.ng/ml; pairwise p < 0.0001).
CONCLUSIONS
MDCO-157, an intravenous formulation of clopidogrel complexed with sulphobutylether betacyclodextrin, did not show significant platelet inhibition when administered at doses up to 300 mg. Higher doses with longer infusion may be needed to reach a sufficient threshold of active metabolite generation.
TRIAL REGISTRATION
ClinicalTrials.gov identifier: NCT01860105.
背景
冠状动脉介入治疗期间P2Y12抑制的程度是缺血性并发症的重要决定因素。目前可用的口服P2Y12抑制剂受到起效相对缓慢和治疗反应个体差异的限制。
目的
我们的目的是确定MDCO - 157(一种与磺丁基醚倍他环糊精复合的氯吡格雷静脉制剂)的药效学(PD)剂量 - 抗血小板反应关系及药代动力学,并确定与口服300mg氯吡格雷的PD效应相匹配的MDCO - 157剂量水平。
方法
在33名健康成年志愿者中进行了一项随机开放标签交叉研究,以确定MDCO - 157剂量为75mg、150mg和300mg以及口服300mg氯吡格雷的药代动力学(氯吡格雷和氯吡格雷H4硫醇活性代谢物)和PD(血管扩张剂刺激的磷蛋白[VASP])效应。
结果
数据以%、均值(标准差)表示。使用VASP通过流式细胞术评估的P2Y12受体抑制的最大效应,静脉注射75mg、150mg和300mg剂量的MDCO - 157分别为70.42(6.7)、69.45(7.1)和65.58(12.6),而口服300mg氯吡格雷为56.6(17.5)(p<0.0001)。静脉注射MDCO - 157导致氯吡格雷的血浆暴露呈逐步增加,高于口服300mg剂量(p<0.0001)。H4 - 硫醇的血浆暴露也随静脉剂量增加(静脉注射75mg、150mg和300mg分别为3.6±2.6、6.9±4.6和12.4±9.1h·ng/ml),但低于口服300mg剂量(34.0±16.0h·ng/ml;两两比较p<0.0001)。
结论
MDCO - 157,一种与磺丁基醚倍他环糊精复合的氯吡格雷静脉制剂,在剂量高达300mg时未显示出显著的血小板抑制作用。可能需要更高剂量和更长输注时间才能达到足够的活性代谢物生成阈值。
试验注册
ClinicalTrials.gov标识符:NCT01860105。
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