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数值方法在可兴奋介质相位缺陷结构检测中的应用。

Numerical methods for the detection of phase defect structures in excitable media.

机构信息

Department of Mathematics, KU Leuven Campus Kortrijk (KULAK), Kortrijk, Belgium.

Laboratory of Experimental Cardiology, Leiden University Medical Center (LUMC), Leiden, The Netherlands.

出版信息

PLoS One. 2022 Jul 12;17(7):e0271351. doi: 10.1371/journal.pone.0271351. eCollection 2022.

Abstract

Electrical waves that rotate in the heart organize dangerous cardiac arrhythmias. Finding the region around which such rotation occurs is one of the most important practical questions for arrhythmia management. For many years, the main method for finding such regions was so-called phase mapping, in which a continuous phase was assigned to points in the heart based on their excitation status and defining the rotation region as a point of phase singularity. Recent analysis, however, showed that in many rotation regimes there exist phase discontinuities and the region of rotation must be defined not as a point of phase singularity, but as a phase defect line. In this paper, we use this novel methodology and perform a comparative study of three different phase definitions applied to in silico data and to experimental data obtained from optical voltage mapping experiments on monolayers of human atrial myocytes. We introduce new phase defect detection algorithms and compare them with those that appeared in literature already. We find that the phase definition is more important than the algorithm to identify sudden spatial phase variations. Sharp phase defect lines can be obtained from a phase derived from local activation times observed during one cycle of arrhythmia. Alternatively, similar quality can be obtained from a reparameterization of the classical phase obtained from observation of a single timeframe of transmembrane potential. We found that the phase defect line length was (35.9 ± 6.2)mm in the Fenton-Karma model and (4.01 ± 0.55)mm in cardiac human atrial myocyte monolayers. As local activation times are obtained during standard clinical cardiac mapping, the methods are also suitable to be applied to clinical datasets. All studied methods are publicly available and can be downloaded from an institutional web-server.

摘要

在心脏中旋转的电波会引发危险的心律失常。找到这种旋转发生的区域是心律失常管理中最重要的实际问题之一。多年来,寻找此类区域的主要方法是所谓的相位映射,其中根据心脏的兴奋状态为点分配连续相位,并将旋转区域定义为相位奇点。然而,最近的分析表明,在许多旋转状态下存在相位不连续性,旋转区域必须定义为相位缺陷线,而不是相位奇点。在本文中,我们使用这种新方法,并对三种不同的相位定义进行了比较研究,这些定义应用于计算机模拟数据和从单层人心房肌细胞光学电压映射实验中获得的实验数据。我们引入了新的相位缺陷检测算法,并将其与已经在文献中出现的算法进行了比较。我们发现,相位定义比识别突然的空间相位变化的算法更重要。从在心律失常的一个周期中观察到的局部激活时间得出的相位,可以获得尖锐的相位缺陷线。或者,可以从观察跨膜电位的单个时间帧获得的经典相位的重新参数化中获得类似的质量。我们发现,在 Fenton-Karma 模型中,相位缺陷线长度为(35.9±6.2)mm,在人心房肌细胞单层中为(4.01±0.55)mm。由于在标准临床心脏映射过程中获得了局部激活时间,因此这些方法也适用于临床数据集。所有研究的方法都是公开的,可以从机构的网络服务器下载。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b70/9275727/fac242c0a5cc/pone.0271351.g001.jpg

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