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A mouse bleeding model to study oral anticoagulants

机译:研究口服抗凝剂的小鼠出血模型

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摘要

New oral anticoagulants to reduce the incidence of thrombosis have recently become available. When compared to the existing therapy, warfarin, these novel agents have similar efficacy with a reduced risk of spontaneous bleeding. However, these novel agents have been associated with significant, even fatal, bleeding following trauma. Reversal agents are being developed that bind and neutralize these oral anticoagulants. However, these are not yet available. Another strategy is to increase thrombin generation by administration of "bypassing" agents such as prothrombin complex concentrates or factor VIIa. Several animal models have been used to model the hemostatic defect induced by the thrombin inhibitor dabigatran. A rat tail injury model, a rabbit cuticle bleeding model, and a rabbit kidney laceration model have all been reported to show increased bleeding, but with supratherapeutic doses of dabigatran. A mouse tail transection model has been reported to reflect increased bleeding at peak therapeutic dabigatran levels. We found that the Whinna saphenous vein hemostasis model reliably reflects a hemostatic defect at therapeutic levels of dabigatran. This model can potentially reflect the effects of reversal or bypassing agents.
机译:最近已经有新的口服抗凝剂可以减少血栓形成的发生。与现有疗法华法林相比,这些新型药物具有相似的功效,并具有减少自发性出血的风险。但是,这些新型药物与创伤后的严重甚至致命的出血有关。正在开发结合并中和这些口服抗凝剂的逆转剂。但是,这些尚不可用。另一种策略是通过施用“绕过”试剂例如凝血酶原复合物浓缩物或因子VIIa来增加凝血酶的产生。已经使用了几种动物模型来模拟凝血酶抑制剂达比加群引起的止血缺陷。据报道,大鼠尾巴损伤模型,兔角质层出血模型和兔肾脏裂伤模型均显示出血增加,但使用达比加群治疗剂量。据报道,小鼠尾部横切模型在达比加群治疗水平达到峰值时出血增加。我们发现,Whinna大隐静脉止血模型可以可靠地反映达比加群治疗水平的止血缺陷。该模型可以潜在地反映反向代理或旁路代理的影响。

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