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关于顺行性旁路位置对预激综合征12导联心电图影响的计算研究

A computational study on the influence of antegrade accessory pathway location on the 12-lead electrocardiogram in Wolff-Parkinson-White syndrome.

作者信息

Gillette Karli, Winkler Benjamin, Kurath-Koller Stefan, Scherr Daniel, Vigmond Edward J, Bär Markus, Plank Gernot

机构信息

Division of Biophysics and Medical Physics, Gottfried Schatz Research Center, Medical University of Graz, Neue Stiftingtalstraße 6, 8010 Graz, Austria.

BioTechMed-Graz, Mozartgasse 12/II, 8010 Graz, Austria.

出版信息

Europace. 2025 Feb 5;27(2). doi: 10.1093/europace/euae223.

Abstract

AIMS

Wolff-Parkinson-White (WPW) syndrome is a cardiovascular disease characterized by abnormal atrioventricular conduction facilitated by accessory pathways (APs). Invasive catheter ablation of the AP represents the primary treatment modality. Accurate localization of APs is crucial for successful ablation outcomes, but current diagnostic algorithms based on the 12-lead electrocardiogram (ECG) often struggle with precise determination of AP locations. In order to gain insight into the mechanisms underlying localization failures observed in current diagnostic algorithms, we employ a virtual cardiac model to elucidate the relationship between AP location and ECG morphology.

METHODS AND RESULTS

We first introduce a cardiac model of electrophysiology that was specifically tailored to represent antegrade APs in the form of a short atrioventricular bypass tract. Locations of antegrade APs were then automatically swept across both ventricles in the virtual model to generate a synthetic ECG database consisting of 9271 signals. Regional grouping of antegrade APs revealed overarching morphological patterns originating from diverse cardiac regions. We then applied variance-based sensitivity analysis relying on polynomial chaos expansion on the ECG database to mathematically quantify how variation in AP location and timing relates to morphological variation in the 12-lead ECG. We utilized our mechanistic virtual model to showcase the limitations of AP localization using standard ECG-based algorithms and provide mechanistic explanations through exemplary simulations.

CONCLUSION

Our findings highlight the potential of virtual models of cardiac electrophysiology not only to deepen our understanding of the underlying mechanisms of WPW syndrome but also to potentially enhance the diagnostic accuracy of ECG-based algorithms and facilitate personalized treatment planning.

摘要

目的

预激综合征(WPW)是一种心血管疾病,其特征是由旁路(APs)促进的房室传导异常。APs的侵入性导管消融是主要的治疗方式。准确确定APs的位置对于成功的消融结果至关重要,但目前基于12导联心电图(ECG)的诊断算法在精确确定APs位置方面常常存在困难。为了深入了解当前诊断算法中观察到的定位失败的潜在机制,我们采用虚拟心脏模型来阐明AP位置与ECG形态之间的关系。

方法与结果

我们首先引入了一种心脏电生理模型,该模型专门设计用于以短房室旁路的形式表示顺行APs。然后在虚拟模型中自动扫描顺行APs在两个心室中的位置,以生成一个由9271个信号组成的合成ECG数据库。顺行APs的区域分组揭示了源自不同心脏区域的总体形态模式。然后,我们对ECG数据库应用基于多项式混沌展开的基于方差的敏感性分析,以数学方式量化AP位置和时间的变化与12导联ECG形态变化之间的关系。我们利用我们的机械虚拟模型展示了使用基于标准ECG的算法进行AP定位的局限性,并通过示例模拟提供了机械解释。

结论

我们的研究结果突出了心脏电生理虚拟模型的潜力,不仅可以加深我们对WPW综合征潜在机制的理解,还可以潜在地提高基于ECG的算法的诊断准确性,并促进个性化治疗计划。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22c8/11879338/130e4e8b8fa9/euae223f1.jpg

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