Danhof M, de Boer A, Magnani H N, Stiekema J C
Center for Bio-Pharmaceutical Sciences, University of Leiden, The Netherlands.
Haemostasis. 1992;22(2):73-84. doi: 10.1159/000216298.
Pharmacokinetic investigations on Orgaran (Org 10172) have been conducted by monitoring the following biological effects: plasma anti-Xa, anti-IIa and IIa-generation-inhibiting (IIaGI) activities. In addition, a limited number of studies were conducted on the basis of concentrations of the No-affinity glycosaminoglyc(uron)an (NoA-GAG) fraction as determined by a competitive binding assay. In humans, widely different pharmacokinetic profiles for various biological effects were observed, with relatively short elimination half-lives for the anti-IIa and IIaGI activities of 4.3 +/- 3.5 and 6.7 +/- 3.2 h, respectively, but a relatively long elimination half-life of anti-Xa activity of 24.5 +/- 9.6 h. These differences in half-life mainly reflect differences in the rate of elimination of individual components of Orgaran. Rapid elimination of some of these components may explain why twice daily dosing is required for optimal thrombosis prophylaxis with Orgaran. In a comparative study in healthy male volunteers, the pharmacokinetics of the following low molecular weight heparin(oid)s were determined after intravenous administration: Orgaran (3,750 anti-Xa units), Fragmin (5,000 anti-Xa units), Fraxiparine (7,500 IC units) and Clexane (40 mg). Between these products, wide differences in pharmacokinetics were observed. Particularly, the half-lives of anti-Xa activity and IIaGI activity were much longer for Orgaran than for the other products. At the same time, a relatively low area under the curve of anti-IIa activity was observed. The absolute bioavailability of Orgaran following subcutaneous administration was determined on the basis of plasma anti-Xa and IIaGI activities and the NoA-GAG fraction concentrations. Absorption from subcutaneous tissues was found to be close to 100%, which is significantly higher than of heparin; a finding which indicates that the subcutaneous route is reliable for the administration of Orgaran. The elimination of Orgaran components occurs by renal and possibly non-renal routes. With respect to anti-Xa activity, about 50% of the total clearance can be accounted for by urinary excretion. Therefore, in severe renal failure, a reduction of the maintenance dose of Orgaran would seem to be indicated. Studies on the influence of enzyme induction as a result of treatment with pentobarbital suggest that the pharmacokinetics of Lomoparan are relatively insensitive to changes in hepatic function. In a number of studies, the influence of conditions such as age, body weight and drug interactions were studied. Generally, only minor changes in the pharmacokinetic parameters of Orgaran were observed.(ABSTRACT TRUNCATED AT 400 WORDS)
通过监测以下生物学效应开展了对奥加诺(Org 10172)的药代动力学研究:血浆抗Xa、抗IIa以及抑制IIa生成(IIaGI)活性。此外,基于通过竞争性结合测定法测定的非亲和性糖胺聚糖(醛糖)(NoA - GAG)组分浓度进行了有限数量的研究。在人类中,观察到各种生物学效应的药代动力学特征差异很大,抗IIa和IIaGI活性的消除半衰期相对较短,分别为4.3±3.5小时和6.7±3.2小时,但抗Xa活性的消除半衰期相对较长,为24.5±9.�小时。半衰期的这些差异主要反映了奥加诺各个组分消除速率的差异。这些组分中某些的快速消除可能解释了为何使用奥加诺进行最佳血栓预防需要每日给药两次。在一项针对健康男性志愿者的比较研究中,静脉给药后测定了以下低分子量肝素(类肝素)的药代动力学:奥加诺(3750抗Xa单位)、速碧林(5000抗Xa单位)、弗希帕宁(7500国际单位)和克赛(40毫克)。在这些产品之间,观察到药代动力学存在很大差异。特别是,奥加诺的抗Xa活性和IIaGI活性的半衰期比其他产品长得多。同时,观察到抗IIa活性的曲线下面积相对较低。基于血浆抗Xa和IIaGI活性以及NoA - GAG组分浓度测定了奥加诺皮下给药后的绝对生物利用度。发现皮下组织的吸收接近100%,这显著高于肝素;这一发现表明皮下途径对于奥加诺的给药是可靠的。奥加诺组分的消除通过肾脏以及可能的非肾脏途径进行。就抗Xa活性而言,约50%的总清除率可由尿排泄来解释。因此,在严重肾衰竭时,似乎需要降低奥加诺的维持剂量。关于戊巴比妥治疗导致的酶诱导影响的研究表明,洛莫帕兰的药代动力学对肝功能变化相对不敏感。在一些研究中,研究了年龄、体重和药物相互作用等情况的影响。一般来说,仅观察到奥加诺药代动力学参数有微小变化。(摘要截选至400字)
