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低分子量肝素依诺肝素在单次皮下注射20至80毫克剂量的人体中的抗血栓活性和药代动力学。

The antithrombotic activity and pharmacokinetics of enoxaparine, a low molecular weight heparin, in humans given single subcutaneous doses of 20 to 80 mg.

作者信息

Frydman A M, Bara L, Le Roux Y, Woler M, Chauliac F, Samama M M

机构信息

Rhône-Poulenc Santé, Institut de Biopharmacie, Antony, France.

出版信息

J Clin Pharmacol. 1988 Jul;28(7):609-18. doi: 10.1002/j.1552-4604.1988.tb03184.x.

DOI:10.1002/j.1552-4604.1988.tb03184.x
PMID:2851016
Abstract

The pharmacokinetics of enoxaparine, a low molecular weight heparin, was randomly studied in 12 healthy male volunteers. Doses of 20, 40, 60, and 80 mg were injected subcutaneously in randomized cross-over fashion. Anti-IIa and anti-Xa activities (using amidolytic methods), and calcium thrombin time, were measured over 36 hours. The maximum Amax of the anti-IIa and anti-Xa activities appeared 3 to 4 hours after administration. The terminal half-lives of anti-IIa and anti-Xa activities were approximately 2 and 4 hours, respectively, with no significant variation between the different doses. For the anti-Xa activity, there was a highly significant positive correlation between the dose injected and individual values of Amax (r = +0.915; P less than .001) and AUC (r = +0.913; P less than .001). Enoxaparine displays a relatively small apparent volume of distribution (about 7.0 L) and its total body clearance is about 1.25 L/hr. The mean residence time ranges from 4.6 to 7.6 hours. Thus, the pharmacokinetic profile of enoxaparine is characterized by a linear relationship between dose and absorption, a relatively low clearance and long elimination half-life, and a high anti-Xa/anti-IIa ratio.

摘要

对12名健康男性志愿者随机进行了低分子量肝素依诺肝素的药代动力学研究。以随机交叉方式皮下注射20、40、60和80毫克剂量的依诺肝素。在36小时内测定抗IIa和抗Xa活性(采用酰胺水解法)以及钙凝血酶时间。抗IIa和抗Xa活性的最大峰值(Amax)在给药后3至4小时出现。抗IIa和抗Xa活性的终末半衰期分别约为2小时和4小时,不同剂量之间无显著差异。对于抗Xa活性,注射剂量与Amax的个体值(r = +0.915;P < 0.001)和曲线下面积(AUC,r = +0.913;P < 0.001)之间存在高度显著的正相关。依诺肝素的表观分布容积相对较小(约7.0升),其全身清除率约为1.25升/小时。平均驻留时间为4.6至7.6小时。因此,依诺肝素的药代动力学特征为剂量与吸收之间呈线性关系、清除率相对较低且消除半衰期较长,以及抗Xa/抗IIa比值较高。

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