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生物物理模型预测室性心动过速的可诱导性和折返环路形态:临床验证与计算机建模相结合的方法

Biophysical Modeling Predicts Ventricular Tachycardia Inducibility and Circuit Morphology: A Combined Clinical Validation and Computer Modeling Approach.

作者信息

Chen Zhong, Cabrera-Lozoya Rocio, Relan Jatin, Sohal Manav, Shetty Anoop, Karim Rashed, Delingette Herve, Gill Jaswinder, Rhode Kawal, Ayache Nicholas, Taggart Peter, Rinaldi Christopher Aldo, Sermesant Maxime, Razavi Reza

机构信息

Kings College London, London, UK.

Guy's and St. Thomas' Hospital, London, UK.

出版信息

J Cardiovasc Electrophysiol. 2016 Jul;27(7):851-60. doi: 10.1111/jce.12991. Epub 2016 Jun 8.

Abstract

INTRODUCTION

Computational modeling of cardiac arrhythmogenesis and arrhythmia maintenance has made a significant contribution to the understanding of the underlying mechanisms of arrhythmia. We hypothesized that a cardiac model using personalized electro-anatomical parameters could define the underlying ventricular tachycardia (VT) substrate and predict reentrant VT circuits. We used a combined modeling and clinical approach in order to validate the concept.

METHODS AND RESULTS

Non-contact electroanatomic mapping studies were performed in 7 patients (5 ischemics, 2 non-ischemics). Three ischemic cardiomyopathy patients underwent a clinical VT stimulation study. Anatomical information was obtained from cardiac magnetic resonance imaging (CMR) including high-resolution scar imaging. A simplified biophysical mono-domain action potential model personalized with the patients' anatomical and electrical information was used to perform in silico VT stimulation studies for comparison. The personalized in silico VT stimulations were able to predict VT inducibility as well as the macroscopic characteristics of the VT circuits in patients who had clinical VT stimulation studies. The patients with positive clinical VT stimulation studies had wider distribution of action potential duration restitution curve (APD-RC) slopes and APDs than the patient with a negative VT stimulation study. The exit points of reentrant VT circuits encompassed a higher percentage of the maximum APD-RC slope compared to the scar and non-scar areas, 32%, 4%, and 0.2%, respectively.

CONCLUSIONS

VT stimulation studies can be simulated in silico using a personalized biophysical cardiac model. Myocardial spatial heterogeneity of APD restitution properties and conductivity may help predict the location of crucial entry/exit points of reentrant VT circuits.

摘要

引言

心脏心律失常发生和维持的计算模型对理解心律失常的潜在机制做出了重大贡献。我们假设使用个性化电解剖参数的心脏模型可以定义潜在的室性心动过速(VT)基质并预测折返性室性心动过速电路。我们采用了建模与临床相结合的方法来验证这一概念。

方法与结果

对7例患者(5例缺血性,2例非缺血性)进行了非接触式电解剖标测研究。3例缺血性心肌病患者接受了临床室性心动过速刺激研究。从心脏磁共振成像(CMR)获得解剖学信息,包括高分辨率瘢痕成像。使用根据患者解剖学和电学信息个性化的简化生物物理单域动作电位模型进行计算机模拟室性心动过速刺激研究以作比较。个性化的计算机模拟室性心动过速刺激能够预测有临床室性心动过速刺激研究患者的室性心动过速诱发能力以及室性心动过速电路的宏观特征。临床室性心动过速刺激研究阳性的患者与室性心动过速刺激研究阴性的患者相比,动作电位时程恢复曲线(APD-RC)斜率和动作电位时程的分布更宽。与瘢痕和非瘢痕区域相比,折返性室性心动过速电路的出口点分别包含更高百分比的最大APD-RC斜率,即32%、4%和0.2%。

结论

可以使用个性化生物物理心脏模型在计算机上模拟室性心动过速刺激研究。动作电位恢复特性和电导率的心肌空间异质性可能有助于预测折返性室性心动过速电路关键入口/出口点的位置。

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