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[宽QRS波群心动过速的鉴别诊断]

[Differential diagnosis of tachycardia with a broad QRS-complex].

作者信息

Deneke Thomas, Mügge Andreas, Kerber Sebastian, Nentwich Karin, Fochler Franziska, Müller Patrick, Grewe Peter, Halbfass Philipp

机构信息

Klinik für Kardiologie II (Rhythmologie/Elektrophysiologie), Herz- und Gefäßklinik Bad Neustadt, Salzburger Leite 1, 97616, Bad Neustadt, Deutschland,

出版信息

Herzschrittmacherther Elektrophysiol. 2015 Sep;26(3):214-26. doi: 10.1007/s00399-015-0387-1. Epub 2015 Sep 1.

Abstract

INTRODUCTION

The electrocardiographic (ECG) differential diagnosis of tachycardia with a broad QRS complex (BCT) represents a challenge for physicians but is important for adequate treatment and risk evaluation. Differentiated algorithms have been established and can increase the specificity of the diagnosis in individual patients but are often hampered by complexity and yield a pragmatic ECG approach.

METHODS AND RESULTS

Irregular BCTs (irregular R-R distances) despite the patient being hemodynamically stable are almost always due to atrial fibrillation with bundle branch block (pre-existing or functional) or conduction via accessory pathways. In contrast, sustained polymorphic ventricular tachycardia (VT) is always associated with hemodynamic collapse. In regular BCT the following mechanisms must be differentiated: (1) VT, (2) supraventricular tachycardia (SVT) with bundle branch block or (3) SVT with pre-excitation via accessory pathways, e.g. Wolff-Parkinson-White (WPW) syndrome. The presence of an underlying structural heart disease, specifically a history of myocardial infarction is suggestive of VT. For a differentiated analysis in hemodynamically stable patients a 12-lead ECG is essential.

CONCLUSION

Identification of signs of atrioventricular (AV) dissociation or a negative precordial concordance of QRS are indicative of VT. In V1 positive BCTs a positive precordial concordance, QRS width > 140 ms, superiorly directed QRS axis, monophasic or biphasic QRS complexes in V1 and deep S wave in V6 are indications of a VT. In V1 negative BCTs, QRS width > 160 ms, right-sided QRS axis, broad R peak (> 40 ms) in V1/V2, slurred S downstroke in V1/V2 and any Q peak in V6 are all indications of VT as the mechanism.

摘要

引言

宽QRS波心动过速(BCT)的心电图(ECG)鉴别诊断对医生来说是一项挑战,但对于恰当治疗和风险评估很重要。已建立了不同的算法,可提高个体患者诊断的特异性,但常因复杂性而受阻,且产生了一种实用的心电图方法。

方法与结果

尽管患者血流动力学稳定,但不规则的BCT(R-R间期不规则)几乎总是由于伴有束支传导阻滞(既往存在或功能性)的心房颤动或经旁路传导所致。相比之下,持续性多形性室性心动过速(VT)总是与血流动力学崩溃相关。在规则的BCT中,必须区分以下机制:(1)VT,(2)伴有束支传导阻滞的室上性心动过速(SVT)或(3)经旁路(如预激综合征,Wolff-Parkinson-White综合征,WPW)预激的SVT。存在潜在的结构性心脏病,特别是有心肌梗死病史提示为VT。对于血流动力学稳定患者的鉴别分析,12导联心电图至关重要。

结论

识别房室(AV)分离征象或QRS波前壁负向一致性提示为VT。在V1导联QRS波正向的BCT中,QRS波前壁正向一致性、QRS波宽度>140ms、QRS波电轴向上、V1导联QRS波为单相或双相且V6导联有深S波是VT的指征。在V1导联QRS波负向的BCT中,QRS波宽度>160ms、QRS波电轴向右、V1/V2导联R波峰宽>40ms、V1/V2导联S波下降支顿挫及V6导联有任何Q波均提示机制为VT。

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