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Therapeutic plasma concentrations of epsilon aminocaproic acid and tranexamic acid in horses.

机译:马匹中ε氨基己酸和氨甲环酸的治疗血浆浓度

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Background: Antifibrinolytic drugs such as epsilon aminocaproic acid (EACA) and tranexamic acid (TEA) are used to treat various bleeding disorders in horses. Although horses are hypofibrinolytic compared to humans, dosing schemes have been derived from pharmacokinetic studies targeting plasma concentrations in humans. Hypothesis/Objectives: We hypothesized therapeutic plasma concentrations of antifibrinolytic drugs in horses would be significantly lower than in humans. Our objective was to use thromboleastography (TEG) and an in vitro model of hyperfibrinolysis to predict therapeutic concentrations of EACA and TEA in horses and humans. Animals: Citrated plasma collected from 24 random source clinically healthy research horses. Commercial pooled human citrated plasma with normal coagulation parameters was purchased. Methods: Minimum tissue plasminogen activator (tPA) concentration to induce complete fibrinolysis within 10 minutes was determined using serial dilutions of tPA in equine plasma. Results used to create an in vitro hyperfibrinolysis model with equine and human citrated plasma, and the minimum concentrations of EACA and TEA required to completely inhibit fibrinolysis for 30 minutes (estimated therapeutic concentrations) determined using serial dilutions of the drugs. Results: Estimated therapeutic concentrations of EACA and TEA were significantly lower in horses (5.82; 95% CI 3.77-7.86 micro g/mL and 0.512; 95% CI 0.277-0.748 micro g/mL) than in humans (113.2; 95% CI 95.8-130.6 micro g/mL and 11.4; 95% CI 8.62-14.1 micro g/mL). Conclusions and Clinical Importance: Current dosing schemes for EACA and TEA in horses may be as much as 20x higher than necessary, potentially increasing cost of treatment and risk of adverse effects.
机译:背景:抗纤溶药物,例如ε氨基己酸(EACA)和氨甲环酸(TEA)用于治疗马匹的各种出血性疾病。尽管与人类相比,马的纤溶酶降低,但剂量方案已经从针对人体血浆浓度的药代动力学研究中得出。假设/目的:我们假设马匹中抗纤溶药物的治疗性血浆浓度将明显低于人类。我们的目标是使用血栓造影术(TEG)和高纤蛋白溶解的体外模型来预测马和人中EACA和TEA的治疗浓度。动物:从24个随机来源的临床健康研究马匹收集的柠檬化血浆。购买了具有正常凝血参数的商业化混合人柠檬酸盐血浆。方法:使用tPA在马血浆中的系列稀释液,确定在10分钟内诱导完全纤维蛋白溶解的最低组织纤溶酶原激活物(tPA)浓度。用于创建具有马和人柠檬酸血浆的体外高纤蛋白溶解模型的结果,以及使用药物的连续稀释液确定的在30分钟内完全抑制纤溶作用所需的最低EACA和TEA浓度(估计治疗浓度)。结果:马中EACA和TEA的估计治疗浓度明显低于人(113.2; 95%CI)(5.82; 95%CI 3.77-7.86 micro g / mL和0.512; 95%CI 0.277-0.748 micro g / mL) 95.8-130.6微克/毫升和11.4; 95%CI 8.62-14.1微克/毫升)。结论和临床重要性:目前在马中EACA和TEA的给药方案可能比所需剂量高出20倍,可能会增加治疗成本和产生不良反应的风险。

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