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心房颤动患者使用直接口服抗凝剂与苯丙香豆素相比的出血、缺血性卒中和死亡率的比较风险。

Comparative risks of bleeding, ischemic stroke and mortality with direct oral anticoagulants versus phenprocoumon in patients with atrial fibrillation.

作者信息

Ujeyl Mariam, Köster Ingrid, Wille Hans, Stammschulte Thomas, Hein Rebecca, Harder Sebastian, Gundert-Remy Ursula, Bleek Julian, Ihle Peter, Schröder Helmut, Schillinger Gerhard, Zawinell Anette, Schubert Ingrid

机构信息

Drug Commission of the German Medical Association, Herbert-Lewin-Platz 1, 10623, Berlin, Germany.

Department of Psychiatry and Psychotherapy at St. Hedwig Hospital, Charité - Universitätsmedizin Berlin, Berlin, Germany.

出版信息

Eur J Clin Pharmacol. 2018 Oct;74(10):1317-1325. doi: 10.1007/s00228-018-2504-7. Epub 2018 Jun 16.

Abstract

PURPOSE

The pivotal trials for stroke prevention in non-valvular atrial fibrillation (NVAF) compared rivaroxaban, dabigatran, and apixaban with warfarin, as did most claims-based studies. Comparisons with phenprocoumon, the most frequently used vitamin K antagonist (VKA) in Germany, are scarce.

METHODS

Risk of bleeding, ischemic stroke, and all-cause mortality in patients with NVAF were analyzed using data for 2010 to 2014 from a large German claims database. New users of oral anticoagulants from January 2012 to December 2013 were included and observed over 1 year. Baseline characteristics were adjusted using propensity score matching and logistic regression. Several sensitivity analyses were carried out.

RESULTS

Fifty-nine thousand four hundred forty-nine rivaroxaban, 23,654 dabigatran, 4894 apixaban, and 87,997 matched phenprocoumon users were included. Adjusted hazard ratios (95% confidence intervals) compared with phenprocoumon were as follows: hospitalized bleedings: rivaroxaban 1.04 (0.97; 1.11), dabigatran 0.87 (0.77; 0.98), and apixaban 0.65 (0.50; 0.86); ischemic stroke: rivaroxaban 1.05 (0.94; 1.17), dabigatran 1.14 (0.96; 1.35), and apixaban 1.84 (1.20; 2.84); all-cause mortality: rivaroxaban 1.17 (1.11; 1.22), dabigatran 1.04 (0.95; 1.13), and apixaban 1.14 (0.97; 1.34).

CONCLUSIONS

With rivaroxaban, no significant differences were observed compared to phenprocoumon with regard to hospitalized bleedings or ischemic strokes. Dabigatran was associated with fewer bleedings and a similar risk of ischemic strokes compared to phenprocoumon. Apixaban was also associated with fewer bleedings but was unexpectedly associated with more ischemic strokes, possibly reflecting selective prescribing. The association of rivaroxaban with higher all-cause mortality unrelated to bleedings or strokes has been described previously but remains to be explained.

摘要

目的

与大多数基于索赔的研究一样,非瓣膜性心房颤动(NVAF)预防卒中的关键试验将利伐沙班、达比加群和阿哌沙班与华法林进行了比较。与德国最常用的维生素K拮抗剂(VKA)苯丙香豆素的比较却很少见。

方法

利用德国一个大型索赔数据库2010年至2014年的数据,分析NVAF患者的出血风险、缺血性卒中和全因死亡率。纳入2012年1月至2013年12月口服抗凝剂的新使用者,并进行1年的观察。使用倾向评分匹配和逻辑回归调整基线特征。进行了多项敏感性分析。

结果

纳入了59449名利伐沙班使用者、23654名达比加群使用者、4894名阿哌沙班使用者以及87997名匹配的苯丙香豆素使用者。与苯丙香豆素相比,调整后的风险比(95%置信区间)如下:住院出血:利伐沙班1.04(0.97;1.11),达比加群0.87(0.77;0.98),阿哌沙班0.65(0.50;0.86);缺血性卒中:利伐沙班1.05(0.94;1.17),达比加群1.14(0.96;1.35),阿哌沙班1.84(1.20;2.84);全因死亡率:利伐沙班1.17(1.11;1.22),达比加群1.04(0.95;1.13),阿哌沙班1.14(0.97;1.34)。

结论

在住院出血或缺血性卒中方面,利伐沙班与苯丙香豆素相比未观察到显著差异。与苯丙香豆素相比,达比加群与较少的出血相关,且缺血性卒中风险相似。阿哌沙班也与较少的出血相关,但意外地与更多的缺血性卒中相关,这可能反映了选择性处方。利伐沙班与更高的全因死亡率相关,且与出血或卒中无关,此前已有描述,但仍有待解释。

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