首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >Individualized dosing regimen for prothrombin complex concentrate more effective than standard treatment in the reversal of oral anticoagulant therapy: An open, prospective randomized controlled trial.
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Individualized dosing regimen for prothrombin complex concentrate more effective than standard treatment in the reversal of oral anticoagulant therapy: An open, prospective randomized controlled trial.

机译:在逆转口服抗凝治疗方面,凝血酶原复合物浓缩物的个性化给药方案比标准治疗更有效:一项开放,前瞻性随机对照试验。

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摘要

Prothrombin Complex Concentrate (PCC) is indicated for the acute reversal of oral anticoagulation therapy. To compare the efficacy of a "standard" dosage of 20 ml PCC equivalent to about 500 IU factor IX (group A), and an "individualized" dosage based on a target-INR of 2.1 or 1.5, the initial-INR and the patient's body weight (group B), we performed an open, prospective, randomized, controlled trial. The in vivo response and in vivo recovery of factor II, VII, IX and X in these patients on oral anticoagulation was determined. Ninety three patients (group A: 47; group B: 46) with major bleedings or admitted for urgent (surgical) interventions were enrolled. PCC and Vitamin K (10 mg) were administered intravenously. We evaluated the effect of treatment by the decrease of INR and the clinical outcome. The number of patients reaching the target-INR 15 min after the dosage of PCC was significantly higher in the group treated with an "individualized" dosage, compared to the group treated with a standard dose, (89% versus 43%; p<0.001). So, we conclude that for the acute reversal of oral anticoagulant therapy, an "individualized" dosage regimen of PCC based on the target-INR, the initial-INR, and body weight of the patient, is significantly more effective in reaching the target-INR than a "standard" dosage. The in vivo response and in vivo recovery found in this study was higher then in patients with isolated factor deficiencies. This suggests that the pharmacokinetics in patients on oral anticoagulants may be different.
机译:凝血酶原复合物浓缩液(PCC)用于口服抗凝治疗的急性逆转。为了比较等效于约500 IU IX因子的20 ml PCC“标准”剂量(基于A组)和基于目标INR 2.1或1.5,初始INR和患者剂量的“个体化”剂量的疗效体重(B组),我们进行了一项开放,前瞻性,随机对照试验。确定了口服抗凝治疗后这些患者体内因子II,VII,IX和X的体内反应和体内恢复情况。纳入了93例严重出血或因急诊(外科手术)入院的患者(A组:47; B组:46)。静脉内施用PCC和维生素K(10毫克)。我们通过降低INR和临床结果评估了治疗效果。与标准剂量治疗组相比,“个体化”剂量治疗组在PCC剂量治疗15分钟后达到目标INR的患者人数显着更高(89%比43%; p <0.001 )。因此,我们得出结论,对于口服抗凝剂治疗的急性逆转,基于患者的目标INR,初始INR和体重的PCC“个体化”给药方案在达到目标- INR高于“标准”剂量。在这项研究中发现的体内反应和体内恢复要高于孤立因素缺乏的患者。这表明口服抗凝剂患者的药代动力学可能不同。

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