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Investigational treatments of venous thromboembolism.

机译:静脉血栓栓塞的治疗方法。

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The antithrombotic management of venous thromboembolism (VTE) has gone through major developments. Indirect inhibitors such as low molecular weight heparin and the pentasaccharide fondaparinux represent improvements over traditional drugs such as unfractionated heparin for acute treatment of VTE with more targeted approaches, predictable pharmacokinetic profiles and lack of need for monitoring. Vitamin K antagonists, with inherent limitations of multiple food and drug interactions and frequent need for monitoring, remain the only oral anticoagulants approved for long-term secondary thromboprophylaxis in VTE with the removal of the oral direct thrombin inhibitor ximelagatran from the world market due to safety concerns. Newer anticoagulant drugs such as parenteral pentasaccharides (idraparinux and SSR-126517-E), oral direct thrombin inhibitors (dabigatran), oral direct Factor Xa inhibitors (rivaroxaban, apixaban, YM-150 and DU-176b) and tissue factor-Factor VIIa complex inhibitors (NAPc2) are tailor-made to target specific procoagulant complexes and have the potential to greatly expand our antithrombotic armamentarium for both acute and long-term treatment of VTE, especially as non-monitored parenteral and oral anticoagulants with a wide therapeutic window and a predictable anticoagulant response.
机译:静脉血栓栓塞症(VTE)的抗血栓形成管理已取得重大进展。间接抑制剂(如低分子量肝素和五糖磺达肝素)代表了对传统药物(如普通肝素)的改进,可通过更有针对性的方法,可预测的药代动力学和无需监测来对VTE进行急性治疗。维生素K拮抗剂具有多种食品和药物相互作用的固有局限性,并且经常需要进行监测,因此由于安全性原因,从世界市场上撤出口服直接凝血酶抑制剂西美加群时,维生素K拮抗剂仍然是批准用于VTE的长期继发性血栓预防的唯一口服抗凝剂关注。较新的抗凝药物,例如肠胃外五糖(idraparinux和SSR-126517-E),口服直接凝血酶抑制剂(达比加群),口服直接Xa因子抑制剂(利伐沙班,阿哌沙班,YM-150和DU-176b)和组织因子-VIIa复合物抑制剂(NAPc2)是针对特定的促凝血复合物量身定制的,具有极大地扩展我们的抗血栓药库的潜力,可用于VTE的急性和长期治疗,尤其是作为非监测型肠胃外和口服抗凝剂,具有宽广的治疗范围和可预测的抗凝反应。

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