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REVIEW: New Antithrombotics for Atrial Fibrillation.

机译:评论:心房颤动的新型抗血栓药。

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Atrial fibrillation (AF) is the most commonly occurring arrhythmia, and is a condition of both significant clinical and economic importance. An antithrombotic agent is considered mandatory as part of the management in most patients with AF. It has been conclusively demonstrated that long-term anticoagulation therapy can significantly reduce the risk of stroke in patients with nonvalvular AF. While vitamin K antagonists (VKAs) such as warfarin are highly effective, they possess numerous limitations that curtail their use, or make their use challenging for clinicians and patients. A new generation of anticoagulants are being investigated in phase III clinical trials in patients with AF. One or more of these agents have the potential to either replace or act as alternatives to VKA therapy in AF. This group includes the direct thrombin inhibitor, dabigatran, the direct factor Xa inhibitors rivaroxaban, apixaban, and edoxaban, and finally, the vitamin K analogue, tecarfarin. Additional agents are being developed in phase I or II clinical trials. The direct thrombin and factor Xa inhibitors are generally small, synthetic molecules with predictable pharmacokinetics, a predictable pharmacodynamic effect, few drug interactions and do not require routine therapeutic drug monitoring. These new anticoagulants may well represent a new era in anticoagulation. However, they do possess their own limitations and will present new challenges for clinicians.
机译:心房颤动(AF)是最常见的心律不齐,并且是具有重要临床和经济意义的疾病。在大多数房颤患者中,抗栓剂被认为是治疗的一部分。最终证明,长期抗凝治疗可以显着降低非瓣膜性房颤患者中风的风险。尽管诸如华法林的维生素K拮抗剂(VKA)非常有效,但它们具有许多局限性,从而限制了其使用或对临床医生和患者造成挑战。在房颤患者的III期临床试验中,正在研究新一代的抗凝剂。这些药物中的一种或多种有可能替代或替代AF中的VKA治疗。此组包括直接凝血酶抑制剂,达比加群,直接因子Xa抑制剂利伐沙班,阿哌沙班和依多沙班,最后是维生素K类似物替卡法林。其他药物正在I或II期临床试验中开发。直接凝血酶和Xa因子抑制剂通常是小的,合成分子,具有可预测的药代动力学,可预测的药效学作用,很少的药物相互作用,并且不需要常规的治疗药物监测。这些新的抗凝剂很可能代表了抗凝的新时代。但是,它们确实有其自身的局限性,并且将为临床医生带来新的挑战。

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