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首页> 外文期刊>Current vascular pharmacology >Bleeding, vertebral fractures and vascular calcifications in patients treated with warfarin: hope for lower risks with alternative therapies.
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Bleeding, vertebral fractures and vascular calcifications in patients treated with warfarin: hope for lower risks with alternative therapies.

机译:华法林治疗的患者的出血,椎骨骨折和血管钙化:希望通过其他疗法降低风险。

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Anticoagulant therapy in patients with atrial fibrillation requires careful evaluation because its benefits i.e. prevention of thromboembolism, must be greater than the risk of bleeding. Patients at higher risk of thrombosis are evaluated through specific scores, such as the CHA(2)DS(2)VASc, coupled with scoring systems for assessing bleeding risks, such as the HAS-BLED score. In addition to bleeding, other risks have been associated with the use of warfarin, including an increased susceptibility to vascular calcifications and fractures caused by a reduction in the levels of vitamin K dependent carboxylated enzymes, matrix Gla-protein (MGP) and bone Gla-protein or osteocalcin (BGP). In fact, while on one side warfarin is used to prevent embolism, on the other hand acting as a vitamin K antagonist it blocks the inhibitory effect of MGP on vascular calcification. Similarly, patients treated with warfarin carry a greater risk of developing osteoporosis and fractures, due to reduced BGP activity. Recently, a new generation of anticoagulant drugs has been developed, such as dabigatran, a direct thrombin inhibitor, and rivaroxaban, a direct factor-Xa inhibitor. They offer an interesting alternative to warfarin, because they do not require frequent blood tests for monitoring while offering similar results in terms of efficacy. Lacking the inhibitory effect on the vitamin K cycle, the consequent side effects can be avoided. If, compared to warfarin treated patients, a lower incidence of vascular calcifications and fractures will be demonstrated, the advantages over warfarin may be even greater, leading to further benefits in terms of morbidity and mortality.
机译:房颤患者的抗凝治疗需要仔细评估,因为其益处(即预防血栓栓塞)必须大于出血风险。通过特定评分(例如CHA(2)DS(2)VASc)以及评估出血风险的评分系统(例如HAS-BLED评分),对处于血栓形成风险较高的患者进行评估。除出血外,华法林的使用还带来其他风险,包括对血管钙化和骨折的敏感性增加,这是由于维生素K依赖的羧化酶,基质Gla蛋白(MGP)和骨骼Gla-蛋白或骨钙蛋白(BGP)。实际上,虽然华法林一方面用于预防栓塞,但另一方面,它用作维生素K拮抗剂,却阻断了MGP对血管钙化的抑制作用。同样,由于BGP活性降低,使用华法林治疗的患者更容易发生骨质疏松和骨折。最近,已经开发了新一代的抗凝药物,例如直接凝血酶抑制剂达比加群和直接凝血因子Xa抑制剂利伐沙班。它们提供了一种替代华法林的有趣替代方法,因为它们不需要进行频繁的血液检查就可以进行监测,同时在功效方面也可获得类似的结果。由于缺乏对维生素K循环的抑制作用,因此可以避免副作用。如果与华法林治疗的患者相比,如果显示血管钙化和骨折的发生率更低,那么与华法林相比的优势可能更大,从而在发病率和死亡率方面带来更多好处。

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