Antithrombotic treatment with direct‐acting oral anticoagulants in patients with splanchnic vein thrombosis and cirrhosis

医学 拜瑞妥 阿哌沙班 达比加群 门静脉血栓形成 肝硬化 血栓形成 内科学 心房颤动 外科 华法林
作者
Andrea De Gottardi,Jonel Trebicka,Christoph Klinger,Aurélie Plessier,Susana Seijó,Benedetta Terziroli Beretta‐Piccoli,Lorenzo Magenta,David Semela,Elisabetta Buscarini,Philippe Langlet,Jan Görtzen,Ángela Puente,Beat Müllhaupt,C.A. Navascués,Filipe Nery,Pierre Deltenre,Fanny Turón,Cornelius Engelmann,Roopen Arya,Karel Caca
出处
期刊:Liver International [Wiley]
卷期号:37 (5): 694-699 被引量:212
标识
DOI:10.1111/liv.13285
摘要

Direct-acting oral anticoagulants (DOACs) are used in patients with splanchnic vein thrombosis (SVT) and cirrhosis, but evidence for safety and efficacy in this setting is limited. Our aim was to identify indications and reasons for starting or switching to DOACs and to report adverse effects, complications and short-term outcome.Data collection including demographic information, laboratory values, treatment and complications through the Vascular Liver Disease Interest Group Consortium.Forty-five centres (90%) of the consortium completed the initial eCRF. We report here a series of 94 patients from 17 centres. Thirty-six patients (38%) had cirrhosis. Child-Pugh score was 6 (range 5-8), and MELD score 10.2 (range 6-19). Indications for anticoagulation were splanchnic vein thrombosis (75%), deep vein thrombosis (5%), atrial fibrillation (14%) and others (6%). DOACs used were rivaroxaban (83%), dabigatran (11%) and apixaban (6%). Patients were followed up for a median duration of 15 months (cirrhotic) and 26.5 months (non-cirrhotic). Adverse events occurred in 17% of patients and included one case of recurrent portal vein thrombosis and five cases of bleeding. Treatment with DOACs was stopped in three cases. The major reasons for choosing DOACs were no need for monitoring or inadequacy of INR to guide anticoagulation in cirrhotic patients. Renal and liver function did not change during treatment.A consistent number of patients with SVT and/or cirrhosis are currently treated with DOACs, which seem to be effective and safe. These data provide a basis for performing randomized clinical trials of DOACs vs. low molecular weight heparin or vitamin K antagonists.
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