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Direct-Acting Oral Anticoagulants (DOACs) in Cirrhosis and Cirrhosis-Associated Portal Vein Thrombosis

机译:肝硬化和肝硬化相关门静脉血栓形成直接作用口服抗凝血剂(DOACS)

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摘要

Direct-acting oral anticoagulants (DOACs) have provided benefit in patients requiring anticoagulation for certain diseases by decreasing the burden of subcutaneous injections and the requirement for frequent monitoring through regular blood tests, to ensure adequacy of the therapeutic doses. Studies have demonstrated DOACs to be as safe, and in some instance safer, compared with traditional anticoagulants in the general population. However, the studies evaluating DOACs excluded patients with cirrhosis, a condition associated with an increased risk of developing portal vein thrombosis (PVT). Warfarin or low-molecular weight heparin are the standard-of-care treatment for acute PVT in cirrhosis, although there is enthusiasm in a paradigm shift switching to DOACs for the treatment of acute PVT in cirrhosis, particularly since the release of DOAC antidotes. This article reviews the current Food and Drug Administration-approved DOACs, hepatic metabolism of DOACs, pharmacokinetics of DOACs in patients with cirrhosis, safety of DOACs (including bleeding, hepatotoxicity, and pregnancy), current treatment guidelines for PVT in cirrhosis, and studies evaluating the use of DOACs in cirrhosis and for the treatment of PVT in cirrhosis. The potential use of DOACs for PVT primary prophylaxis in at-risk patients with cirrhosis and the possible antifibrotic effects of DOACs are also discussed.
机译:直接作用口服抗凝血剂(DOAC)通过降低皮下注射的负担以及通过定期验血的频繁监测的要求,为某些疾病进行抗凝的患者提供了益处,以确保治疗剂量的充分性。研究表明,与一般人群中的传统抗凝血剂相比,DOACS保持安全,并且在一些实例更安全。然而,评估Doacs的研究排除了肝硬化患者,一种与发育门静脉血栓形成(PVT)的风险增加相关的病症。 Warfarin或低分子量肝素是肝硬化中急性PVT的标准治疗方法,尽管在肝硬化中治疗急性PVT的抗原型转变切换的急性PVT的热情,特别是因为DOAC解毒剂释放以来。本文审查了当前的食品和药物管理局批准的Doacs,Doacs的肝脏代谢,肝硬化患者的Doacs药代动力学,Doacs的安全性(包括出血,肝毒性和妊娠),目前的肝硬化的PVT治疗准则以及研究评估肝硬化中的DOACS在肝硬化中的治疗PVT。还讨论了患有肝硬化患者患者的PVT主要预防的DoAC和Doacs可能的抗灰度作用的潜在使用。

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