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直接凝血酶抑制剂(阿加曲班、比伐卢定和来匹卢定)和间接 Xa 因子抑制剂(达那肝素)增加纤维蛋白网络的孔隙率,从而促进纤维蛋白溶解。

The direct thrombin inhibitors (argatroban, bivalirudin and lepirudin) and the indirect Xa-inhibitor (danaparoid) increase fibrin network porosity and thus facilitate fibrinolysis.

机构信息

Department of Clinical Sciences, Danderyd Hospital, Karolinska Institutet, Stockholm, Sweden.

出版信息

Thromb Haemost. 2010 May;103(5):1076-84. doi: 10.1160/TH09-05-0306. Epub 2010 Mar 9.

DOI:10.1160/TH09-05-0306
PMID:20216982
Abstract

The present study aimed to assess whether the fibrin network structure is modified by the direct thrombin-inhibitors lepirudin, argatroban or bivalirudin and by the indirect Xa-inhibitor danaparoid. Using an in vitro assay that imitates the physiological process of coagulation from thrombin generation to fibrin formation, we examined a normal plasma pool spiked with one of the inhibitors. At concentrations considered to be the plasma levels observed during therapy, almost no influence was detected for lepirudin despite clear-cut effects on "clotting time". However, argatroban, bivalirudin and danaparoid increased the fibrin gel permeability (Ks) to a similar extent. At concentrations higher than the "therapeutic" levels, the dose-response curve in the Ks assay became very steep for lepirudin while those were shallow for the others. In parallel with the drug-induced increases of Ks, larger network pores in 3D-microscopic images and significant shortenings in "clot lysis time" induced by addition of rtPA were observed. Recombinant factor VIII (rFVIII) added to danaparoid-treated samples profoundly counteracted the increase of Ks but had only a slight or no effect on the other drugs. Thus, in vitro, argatroban, bivalirudin and danaparoid have comparable anticoagulating effects, rendering the fibrin network more permeable and less resistant to fibrinolysis. For lepirudin, the steep dose-response curve supports previous clinical findings, i.e. this thrombin inhibitor has a narrow therapeutic window. Furthermore, our data suggest that the haemostatic agent, rFVIII, might be effective in treatment of bleeding complications induced by danaparoid.

摘要

本研究旨在评估直接凝血酶抑制剂 lepirudin、argatroban 或 bivalirudin 以及间接 Xa 抑制剂 danaparoid 是否会改变纤维蛋白网络结构。我们使用一种体外测定法,模拟从凝血酶生成到纤维蛋白形成的生理凝血过程,检测了加入一种抑制剂的正常血浆池。在考虑到治疗期间观察到的血浆水平的浓度下,尽管对“凝血时间”有明显影响,但 lepirudin 几乎没有影响。然而,argatroban、bivalirudin 和 danaparoid 会以相似的程度增加纤维蛋白凝胶的通透性(Ks)。在高于“治疗”水平的浓度下,Ks 测定中的剂量-反应曲线对 lepirudin 变得非常陡峭,而对其他药物则较浅。与药物诱导的 Ks 增加平行,在添加 rtPA 时,在 3D 显微镜图像中观察到更大的网络孔和明显缩短的“血凝块溶解时间”。添加到 danaparoid 处理的样品中的重组因子 VIII (rFVIII) 显著抵消了 Ks 的增加,但对其他药物只有轻微或没有影响。因此,在体外,argatroban、bivalirudin 和 danaparoid 具有相似的抗凝作用,使纤维蛋白网络更具通透性且对纤维蛋白溶解的抵抗力降低。对于 lepirudin,陡峭的剂量-反应曲线支持先前的临床发现,即这种凝血酶抑制剂的治疗窗口较窄。此外,我们的数据表明,止血剂 rFVIII 可能有效治疗由 danaparoid 引起的出血并发症。

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