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心室解剖结构的复杂性和性别差异会影响电生理计算模型的预测。

Ventricular anatomical complexity and sex differences impact predictions from electrophysiological computational models.

机构信息

ELEM Biotech S.L., Barcelona, Spain.

Barcelona Supercomputing Center, Barcelona, Spain.

出版信息

PLoS One. 2023 Feb 13;18(2):e0263639. doi: 10.1371/journal.pone.0263639. eCollection 2023.

Abstract

The aim of this work was to analyze the influence of sex hormones and anatomical details (trabeculations and false tendons) on the electrophysiology of healthy human hearts. Additionally, sex- and anatomy-dependent effects of ventricular tachycardia (VT) inducibility are presented. To this end, four anatomically normal, human, biventricular geometries (two male, two female), with identifiable trabeculations, were obtained from high-resolution, ex-vivo MRI and represented by detailed and smoothed geometrical models (with and without the trabeculations). Additionally one model was augmented by a scar. The electrophysiology finite element model (FEM) simulations were carried out, using O'Hara-Rudy human myocyte model with sex phenotypes of Yang and Clancy. A systematic comparison between detailed vs smooth anatomies, male vs female normal hearts was carried out. The heart with a myocardial infarction was subjected to a programmed stimulus protocol to identify the effects of sex and anatomical detail on ventricular tachycardia inducibility. All female hearts presented QT-interval prolongation however the prolongation interval in comparison to the male phenotypes was anatomy-dependent and was not correlated to the size of the heart. Detailed geometries showed QRS fractionation and increased T-wave magnitude in comparison to the corresponding smoothed geometries. A variety of sustained VTs were obtained in the detailed and smoothed male geometries at different pacing locations, which provide evidence of the geometry-dependent differences regarding the prediction of the locations of reentry channels. In the female phenotype, sustained VTs were induced in both detailed and smooth geometries with RV apex pacing, however no consistent reentry channels were identified. Anatomical and physiological cardiac features play an important role defining risk in cardiac disease. These are often excluded from cardiac electrophysiology simulations. The assumption that the cardiac endocardium is smooth may produce inaccurate predictions towards the location of reentry channels in in-silico tachycardia inducibility studies.

摘要

本研究旨在分析性激素和解剖学细节(小梁和假性腱索)对健康人心肌电生理的影响。此外,还介绍了室性心动过速(VT)诱导的性别和解剖依赖性效应。为此,从高分辨率的离体 MRI 中获得了四个解剖正常的人类双心室几何形状(两个男性,两个女性),可识别小梁,并通过详细和光滑的几何模型(带小梁和不带小梁)进行表示。此外,一个模型还增加了一个疤痕。使用具有 Yang 和 Clancy 性别表型的 O'Hara-Rudy 人心肌细胞模型进行了电生理学有限元模型(FEM)模拟。对详细解剖与光滑解剖、男性与女性正常心脏进行了系统比较。对心肌梗死心脏进行程控刺激方案,以确定性别和解剖细节对室性心动过速诱导的影响。所有女性心脏均出现 QT 间期延长,但与男性表型相比,延长间隔取决于解剖结构,与心脏大小无关。与相应的光滑几何形状相比,详细几何形状显示 QRS 碎裂和 T 波幅度增加。在不同起搏部位,在详细和光滑的男性几何形状中获得了各种持续的 VT,这为关于折返通道预测位置的几何形状依赖性差异提供了证据。在女性表型中,在 RV 心尖起搏时,在详细和光滑的几何形状中均诱导出持续的 VT,但未识别出一致的折返通道。心脏解剖和生理特征在心脏疾病风险的定义中起着重要作用。这些特征通常在心脏电生理学模拟中被排除在外。假设心脏心内膜是光滑的,可能会在心脏电生理模拟中对折返通道的位置产生不准确的预测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bd1/9925004/746589c67ec1/pone.0263639.g001.jpg

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