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随机接受依度沙班或华法林治疗的房颤患者的死亡率:ENGAGE AF-TIMI 48试验的见解。

Mortality in Patients with Atrial Fibrillation Randomized to Edoxaban or Warfarin: Insights from the ENGAGE AF-TIMI 48 Trial.

作者信息

Giugliano Robert P, Ruff Christian T, Wiviott Stephen D, Nordio Francesco, Murphy Sabina A, Kappelhof Johannes A N, Shi Minggao, Mercuri Michele F, Antman Elliott M, Braunwald Eugene

机构信息

TIMI Study Group, Cardiovascular Medicine, Brigham and Women's Hospital, Boston, Mass.

TIMI Study Group, Cardiovascular Medicine, Brigham and Women's Hospital, Boston, Mass.

出版信息

Am J Med. 2016 Aug;129(8):850-857.e2. doi: 10.1016/j.amjmed.2016.02.028. Epub 2016 Mar 17.

Abstract

BACKGROUND

When compared with warfarin, edoxaban significantly reduced cardiovascular mortality in the Effective Anticoagulation with Factor Xa Next Generation in Atrial Fibrillation-Thrombolysis in Myocardial Infarction 48 (ENGAGE AF-TIMI 48) trial. We studied the possible reasons leading to this reduction.

METHODS

ENGAGE AF-TIMI 48 was a double-blind, double-dummy comparison of warfarin with 2 regimens of once-daily edoxaban in 21,105 patients with atrial fibrillation followed for 2.8 years (median). Causes of deaths in the intention-to-treat population were classified as cardiovascular (including fatal bleeding and ischemic stroke), malignancy, or noncardiovascular/nonmalignancy by an independent, blinded, clinical endpoint committee. Deaths also were adjudicated as directly due to bleeding (ie, fatal), or bleeding contributing to death, or neither.

RESULTS

There were 839 total deaths (4.35%/y) in the warfarin arm, compared with 773 (3.99%/y, P = .08) with the higher-dose edoxaban regimen, and 737 (3.80%/y, P = .006) with the lower-dose edoxaban regimen. No significant differences between treatments were observed in (1) any of the 3 most common causes of cardiovascular death (sudden cardiac, heart failure, ischemic stroke), (2) fatal malignancies, (3) other noncardiovascular death. There were 124 fatal bleeds, 65 with warfarin, significantly fewer with the higher-dose (n = 35, P = .003) and lower-dose (n = 24, P < .001) edoxaban regimens. There were 101 bleeding events with warfarin that were either fatal or that contributed to death. There were significantly fewer with the higher-dose (n = 59, P = .001) and lower-dose (n = 54, P < .001) edoxaban regimens.

CONCLUSIONS

Fewer total and cardiovascular deaths were observed with edoxaban as compared with warfarin in the ENGAGE AF-TIMI 48 trial, and this predominantly resulted from the significantly lower rate of major bleeding with edoxaban. Edoxaban reduces mortality both directly (less fatal bleeding) and indirectly (fewer bleeding-related complications and interruptions in therapy after nonfatal bleeding).

摘要

背景

在房颤患者中进行的依度沙班与华法林有效性比较的“依度沙班用于房颤治疗-心肌梗死溶栓48研究(ENGAGE AF-TIMI 48)”试验中,与华法林相比,依度沙班显著降低了心血管死亡率。我们研究了导致这种降低的可能原因。

方法

ENGAGE AF-TIMI 48是一项双盲、双模拟试验,在21105例房颤患者中比较华法林与两种每日一次依度沙班方案,随访时间中位数为2.8年。意向性治疗人群的死亡原因由一个独立、盲法的临床终点委员会分类为心血管原因(包括致命性出血和缺血性卒中)、恶性肿瘤或非心血管/非恶性肿瘤。死亡也被判定为直接因出血(即致命性)、出血促成死亡或两者皆非。

结果

华法林组共有839例死亡(4.35%/年),高剂量依度沙班方案组有773例死亡(3.99%/年,P = 0.08),低剂量依度沙班方案组有737例死亡(3.80%/年,P = 0.006)。在以下方面未观察到治疗组之间的显著差异:(1)心血管死亡的3种最常见原因(心源性猝死、心力衰竭、缺血性卒中)中的任何一种;(2)致命性恶性肿瘤;(3)其他非心血管死亡。有124例致命性出血,华法林组65例,高剂量依度沙班方案组显著更少(n = 35,P = 0.003),低剂量依度沙班方案组也显著更少(n = 24,P < 0.001)。华法林组有101例出血事件,这些事件要么是致命性的,要么促成了死亡。高剂量依度沙班方案组(n = 59,P = 0.001)和低剂量依度沙班方案组(n = 54,P < 0.001)的此类事件显著更少。

结论

在ENGAGE AF-TIMI 48试验中,与华法林相比,依度沙班的总死亡和心血管死亡更少,这主要是由于依度沙班的大出血发生率显著更低。依度沙班通过直接(更少致命性出血)和间接(更少出血相关并发症以及非致命性出血后治疗中断)两种方式降低死亡率。

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