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Non-invasive assessment of spatiotemporal organization of ventricular fibrillation through principal component analysis

机译:通过主成分分析非侵入性评估室颤的时空组织

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Introduction Ventricular fibrillation (VF) is the main cause of sudden cardiac death, but we lack tools to predict the evolution of its complexity. This study proposes novel VF complexity markers obtained by principal component analysis (PCA) of body surface potential maps (BSPMs). Methods BSPMs were divided in 0.5-s segments, each projected on the 3D PCA subspace determined in the previous frame. Reconstruction error ϵ was expressed in terms of norm dϵand angle cosine cos(αϵ), and the nondipolar component index (NDI) quantified the energy of the first 3 PCA eigenvalues. These markers quantified changes in complexity between the beginning and the end of 24 VF episodes and 5 control sinus rhythm (SR) recordings. They were also tested on 6 BSPMs from a torso-tank model during and after ex-vivo pig heart perfusion. Differences between in-silico BSPM right and left leads were then verified in 4 human VF simulations, with a reentrant source in the right ventricle. Results Higher NDI and dϵand lower cos(αϵ) denoted higher complexity at the end of VF (p <; 0.0001). No changes occurred in SR (p > 0.05). The indices also underlined higher disorganization in ex-vivo non-perfused VF (p <; 0.0001). A similar trend was observed in the right in-silico BSPM leads (p <; 0.05). Conclusions PCA can non-invasively quantify changes in VF complexity.
机译:简介心室纤颤(VF)是心源性猝死的主要原因,但我们缺乏预测其复杂性演变的工具。这项研究提出了新的VF复杂性标记,通过体表电位图(BSPM)的主成分分析(PCA)获得。方法将BSPM分为0.5 s的段,每个段都投影在前一帧中确定的3D PCA子空间上。重建误差ϵ用范数d表示 ϵ 和角余弦余弦(α ϵ ),并且非偶极分量指数(NDI)量化了前3个PCA特征值的能量。这些标记物量化了24个VF发作和5个控制窦性心律(SR)记录的开始和结束之间的复杂性变化。在离体猪心脏灌注期间和之后,还对来自躯干坦克模型的6种BSPM进行了测试。然后在4个人类VF模拟中验证了硅内BSPM右导线和左导线之间的差异,右室中有一个折返源。结果更高的NDI和d ϵ 和较低的cos(α ϵ )表示VF结束时具有更高的复杂度(p <; 0.0001)。 SR没有发生变化(p> 0.05)。该指数还强调了离体非灌注VF的更高的无序性(p <; 0.0001)。在正确的计算机内BSPM引线中观察到了类似的趋势(p <; 0.05)。结论PCA可以无创地量化VF复杂性的变化。

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