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使用阿加曲班治疗有肝素诱导的血小板减少症病史且存在抗重组水蛭素抗体的患者。

Treatment of patients with a history of heparin-induced thrombocytopenia and anti-lepirudin antibodies with argatroban.

作者信息

Harenberg Job, Jörg Ingrid, Fenyvesi Tivadar, Piazolo Lukas

机构信息

IV. Department of Medicine, University Hospital Mannheim, Ruprecht-Karls-University Heidelberg, Theodor-Kutzer-Ufer 1-3, D-68167 Mannheim, Germany.

出版信息

J Thromb Thrombolysis. 2005 Feb;19(1):65-9. doi: 10.1007/s11239-005-0942-4.

Abstract

Patients with heparin-induced thrombocytopenia (HIT) type II require anticoagulation with non-heparin immediate acting anticoagulants. Danaparoid may cross react with HIT-antibodies and lepirudin may generate anti-lepirudin antibodies influencing anticoagulation. We hypothesised, that the synthetic small molecular thrombin inhibitor argatroban does not induce immunoglobulins reacting towards lepirudin in patients with anti-lepirudin antibodies in the history and that titration of the anticoagulation may be easier with argatroban. We report on the treatment of four patients of a study, which was terminated prematurely due to official warnings for a repeated use of lepirudin. Two patients each received argatroban and lepirudin intravenously. A blinded assessor adjusted the doses of the anticoagulants to 1.5-3.0 fold prolongation of the aPTT. Ecarin clotting time (ECT), concentrations of lepirudin (ELISA) and of argatroban (gas-chromatography with mass spectrometry), and the generation of lepirudin antibodies (ELISA) were measured. APTT-adjusted dosages for argatroban was 2.0-2.6 microg/kg.min and for lepirudin 48-149 microg/kg.h. ECT was prolonged 2.1 to 4.5-fold with lepirudin and 4 to 7-fold with argatroban. The concentration of lepirudin ranged between 750 and 1500 ng/ml and of argatroban between 400 and 1100 ng/ml. Patients on argatroban did not generate immunoglobulin IgG reacting towards lepirudin in contrast to both patients on lepirudin who developed anti-lepirudin antibodies. Both treatments were well tolerated. Despite the low number of patients argatroban seems to lead to a more stable anticoagulant response than lepirudin resulting in a lower variability of the dosage for prophylaxis or treatment of thromboembolism of patients with a history of HIT and lepirudin antibodies.

摘要

II型肝素诱导的血小板减少症(HIT)患者需要使用非肝素速效抗凝剂进行抗凝。达那肝素可能与HIT抗体发生交叉反应,而重组水蛭素可能产生影响抗凝作用的抗重组水蛭素抗体。我们推测,合成的小分子凝血酶抑制剂阿加曲班不会在有抗重组水蛭素抗体病史的患者中诱导产生针对重组水蛭素的免疫球蛋白,并且使用阿加曲班进行抗凝滴定可能更容易。我们报告了一项研究中4例患者的治疗情况,该研究因官方对重复使用重组水蛭素的警告而提前终止。2例患者分别接受了阿加曲班和重组水蛭素静脉注射。一位盲法评估者将抗凝剂剂量调整至活化部分凝血活酶时间(aPTT)延长1.5 - 3.0倍。测量了蛇静脉酶凝血时间(ECT)、重组水蛭素浓度(酶联免疫吸附测定法)和阿加曲班浓度(气相色谱 - 质谱联用),以及重组水蛭素抗体的产生(酶联免疫吸附测定法)。阿加曲班的aPTT调整剂量为2.0 - 2.6微克/千克·分钟,重组水蛭素为48 - 149微克/千克·小时。重组水蛭素使ECT延长2.1至4.5倍,阿加曲班使ECT延长4至7倍。重组水蛭素浓度在750至1500纳克/毫升之间,阿加曲班浓度在400至1100纳克/毫升之间。与接受重组水蛭素治疗且产生抗重组水蛭素抗体的2例患者不同,接受阿加曲班治疗的患者未产生针对重组水蛭素的免疫球蛋白IgG。两种治疗耐受性均良好。尽管患者数量较少,但与重组水蛭素相比,阿加曲班似乎能导致更稳定的抗凝反应,从而使有HIT病史和重组水蛭素抗体的患者在预防或治疗血栓栓塞时剂量变异性更低。

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