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房性早搏作为心房心肌病的标志物:ARCADIA随机试验的修订分析

Premature Atrial Contractions as a Marker of Atrial Cardiopathy: A Revised Analysis of the ARCADIA Randomized Trial.

作者信息

Elias Adi, Teraoka Justin T, Soliman Elsayed Z, Elkind Mitchell S V, Kamel Hooman, Kronmal Richard A, Longstreth W T, Tirschwell David L, Di Tullio Marco R, Marcus Gregory M

机构信息

Division of Cardiology, University of California San Francisco, San Francisco, California, USA.

Department of Cardiovascular Medicine, Wake Forest University School of Medicine, Winston-Salem, North Carolina, USA.

出版信息

J Cardiovasc Electrophysiol. 2025 Jul;36(7):1487-1493. doi: 10.1111/jce.16629. Epub 2025 Apr 28.

Abstract

INTRODUCTION

Atrial cardiopathy may be associated with an increased risk of stroke independent of atrial fibrillation (AF). In the ARCADIA trial, apixaban was not superior to aspirin in preventing recurrent stroke among patients with a cryptogenic stroke and atrial cardiopathy. We aimed to determine whether the presence of at least one premature atrial complex (PAC), a known harbinger of AF and stroke, would enhance the ability to identify individuals most likely to benefit from apixaban.

METHODS

In ARCADIA, atrial cardiopathy was defined by NT-proBNP > 250 pg/mL, a P-wave terminal force greater than 5000 μV × ms in lead V1, or a left atrial diameter index ≥ 3 cm/m² on echocardiogram. For the current analysis, the presence of any PAC on the baseline 12-lead ECG was substituted for the less atrial-specific NT-proBNP criterion. The presence of any PAC was also assessed as a sole atrial cardiopathy criterion.

RESULTS

Of the 1015 patients randomized in ARCADIA, 85 had at least one PAC. The revised atrial cardiopathy criteria were met by 593 patients; 301 were randomized to apixaban and 292 to aspirin. The annualized recurrent stroke rates were 3.1% for apixaban versus 4.4% for aspirin (HR 0.71, 95% CI: 0.38-1.34, p = 0.29). No differences in risk of recurrent stroke among participants with PACs, compared to those without PACs, were observed.

CONCLUSION

In patients enrolled in the ARCARDIA trial, utilizing the presence of PACs as a potential marker of atrial cardiopathy did not reveal definitive evidence of benefit of apixaban compared to aspirin.

TRIAL REGISTRATION

ClinicalTrials.gov identifier: NCT03192215.

摘要

引言

心房心肌病可能与心房颤动(AF)无关的中风风险增加有关。在ARCADIA试验中,在预防隐源性中风和心房心肌病患者的复发性中风方面,阿哌沙班并不优于阿司匹林。我们旨在确定至少一个房性早搏(PAC)的存在(AF和中风的已知先兆)是否会增强识别最有可能从阿哌沙班中获益的个体的能力。

方法

在ARCADIA试验中,心房心肌病的定义为N末端脑钠肽前体(NT-proBNP)>250 pg/mL、V1导联P波终末电势大于5000 μV×ms或超声心动图显示左心房直径指数≥3 cm/m²。对于当前分析,基线12导联心电图上任何PAC的存在替代了特异性较低的NT-proBNP标准。任何PAC的存在也被评估为唯一的心房心肌病标准。

结果

在ARCADIA试验中随机分组的1015例患者中,85例至少有一个PAC。593例患者符合修订后的心房心肌病标准;301例随机接受阿哌沙班治疗,292例接受阿司匹林治疗。阿哌沙班的年化复发性中风率为3.1%,阿司匹林为4.4%(风险比0.71,95%置信区间:0.38 - 1.34,p = 0.29)。与没有PAC的参与者相比,有PAC的参与者在复发性中风风险上没有观察到差异。

结论

在参与ARCADIA试验的患者中,利用PAC的存在作为心房心肌病的潜在标志物,与阿司匹林相比,未发现阿哌沙班有明确获益证据。

试验注册

ClinicalTrials.gov标识符:NCT03192215。

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