通过非线性心率动力学分析识别心血管风险：从小鼠到人类的转化生物标志物。

IF 2.7 3区医学 Q3 NEUROSCIENCES

Brain Sciences Pub Date : 2025-03-14 DOI:10.3390/brainsci15030306

Torben Hager, Agorastos Agorastos, Sven Ove Ögren, Oliver Stiedl

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引用次数: 0

摘要

背景：心率（HR）随搏动时间序列的波动（HR动力学）提供了自主神经系统（ANS）在病理状态下的HR调节及其失调的信息。通常，尽管存在明显的统计和翻译局限性，但仍使用HR及其变异性（HRV）的线性分析来得出病理状态的结论。目的：本研究的主要目的是比较C57BL/6N小鼠基于电遥测记录的线性和非线性心率测量，包括去趋势波动分析（DFA），以确定病理心率动态。方法：我们研究了通过各种外周和/或中枢机制（包括与精神疾病有关的受体）改变ANS调节的不同行为和广泛的药物干预。这一系列干预措施可作为比较线性和非线性HR措施以确定病理状态的参考系统。结果：生理DFA动态是一个自相似的、尺度不变的分形过程，具有持久的内在长程相关性，导致生理DFA标度系数为α~1。DFA标度系数的显著改变（α≠1）表明(1)副交感神经阻滞、(2)副交感神经过度激活和(3)交感神经过度激活而非抑制引起了HR动力学的病理状态。在小鼠和人的生理条件下，通过规定的药物干预，在相同的病理状态下，DFA缩放系数是相同的。结论：在这里，我们展示了紧张性迷走神经功能对小鼠生理HR动力学的重要性，正如在人类中报道的那样。与线性测量不同，DFA提供了一种重要的转化测量，可以可靠地识别基于药物干预改变的ANS控制的病理HR动态。中枢ANS失调可能是精神疾病中心脏死亡率增加的一种机制。

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Identifying Cardiovascular Risk by Nonlinear Heart Rate Dynamics Analysis: Translational Biomarker from Mice to Humans.

Background: The beat-by-beat fluctuation of heart rate (HR) in its temporal sequence (HR dynamics) provides information on HR regulation by the autonomic nervous system (ANS) and its dysregulation in pathological states. Commonly, linear analyses of HR and its variability (HRV) are used to draw conclusions about pathological states despite clear statistical and translational limitations.

Objective: The main aim of this study was to compare linear and nonlinear HR measures, including detrended fluctuation analysis (DFA), based on ECG recordings by radiotelemetry in C57BL/6N mice to identify pathological HR dynamics.

Methods: We investigated different behavioral and a wide range of pharmacological interventions which alter ANS regulation through various peripheral and/or central mechanisms including receptors implicated in psychiatric disorders. This spectrum of interventions served as a reference system for comparison of linear and nonlinear HR measures to identify pathological states.

Results: Physiological HR dynamics constitute a self-similar, scale-invariant, fractal process with persistent intrinsic long-range correlations resulting in physiological DFA scaling coefficients of α~1. Strongly altered DFA scaling coefficients (α ≠ 1) indicate pathological states of HR dynamics as elicited by (1) parasympathetic blockade, (2) parasympathetic overactivation and (3) sympathetic overactivation but not inhibition. The DFA scaling coefficients are identical in mice and humans under physiological conditions with identical pathological states by defined pharmacological interventions.

Conclusions: Here, we show the importance of tonic vagal function for physiological HR dynamics in mice, as reported in humans. Unlike linear measures, DFA provides an important translational measure that reliably identifies pathological HR dynamics based on altered ANS control by pharmacological interventions. Central ANS dysregulation represents a likely mechanism of increased cardiac mortality in psychiatric disorders.

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来源期刊

Brain Sciences Neuroscience-General Neuroscience

CiteScore

4.80

自引率

9.10%

发文量

1472

审稿时长

18.71 days

期刊介绍： Brain Sciences (ISSN 2076-3425) is a peer-reviewed scientific journal that publishes original articles, critical reviews, research notes and short communications in the areas of cognitive neuroscience, developmental neuroscience, molecular and cellular neuroscience, neural engineering, neuroimaging, neurolinguistics, neuropathy, systems neuroscience, and theoretical and computational neuroscience. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. Electronic files or software regarding the full details of the calculation and experimental procedure, if unable to be published in a normal way, can be deposited as supplementary material.