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心室颤动中相位奇点的空间分布。

Spatial distribution of phase singularities in ventricular fibrillation.

作者信息

Valderrábano Miguel, Chen Peng-Sheng, Lin Shien-Fong

机构信息

Division of Cardiology, Department of Medicine, Cedars-Sinai Medical Center and David Geffen School of Medicine, University of California Los Angeles, Calif 90048, USA.

出版信息

Circulation. 2003 Jul 22;108(3):354-9. doi: 10.1161/01.CIR.0000080322.67408.B4. Epub 2003 Jun 30.

Abstract

BACKGROUND

Multiple excitation wavelets are present during ventricular fibrillation (VF). The underlying wavelet organization of VF is unclear. Phase singularities (PSs)-locations of ambiguous activation state-underlie reentry and wavelet splitting and represent the sources of VF. Understanding the mechanisms of PS formation might be important in the development of effective therapies for sudden death.

METHODS AND RESULTS

We performed voltage, phase, and PS mapping in fibrillating ventricles, applying an automated PS detection algorithm to optically recorded fibrillation signals. PS clustering was noted along epicardial vessels, ridges of endocardial trabeculae, and papillary muscle insertions. Microscopically, these locations correlated with areas of apposition of fibers with different angulations and intramural vessels. A total of 83.2% of PSs were formed at and meandered about these anatomic structures, which acted as stabilizers: PSs colocalizing at anatomic substrates had longer life spans than nonanatomic PS (82.46+/-60.8 versus 40.5+/-31.9 ms, P<0.01). The RV endocardium had a higher PS incidence than the epicardium (42.3+/-9.2 versus 23.5+/-11.6 PS/s, P<0.01). Autocorrelation showed that irregular behavior was spatially restricted to anatomic heterogeneities compared with other areas, which had nearly periodic behaviors. Simple spatial PS distributions underlay complex and variable activation patterns attributable to variable PS behaviors, life spans, and inter-PS interactions.

CONCLUSIONS

PSs occur in a nonrandom spatial distribution and colocalize with normal anatomic heterogeneities. Varying PS behaviors and life spans but stable PS spatial distributions cause ever-changing activation patterns that characterize VF.

摘要

背景

心室颤动(VF)期间存在多个激发小波。VF潜在的小波组织尚不清楚。相位奇点(PSs)——模糊激活状态的位置——是折返和小波分裂的基础,代表VF的起源。了解PS形成机制可能对开发有效的猝死治疗方法很重要。

方法与结果

我们在颤动的心室中进行了电压、相位和PS映射,将自动PS检测算法应用于光学记录的颤动信号。在心脏外膜血管、心内膜小梁嵴和乳头肌附着处观察到PS聚集。在显微镜下,这些位置与不同角度纤维和壁内血管的贴合区域相关。总共83.2%的PSs在这些解剖结构处形成并围绕其蜿蜒,这些结构起到了稳定剂的作用:与非解剖学PS相比,共定位在解剖学基质上的PSs具有更长的寿命(82.46±60.8对40.5±31.9毫秒,P<0.01)。右心室心内膜的PS发生率高于心脏外膜(42.3±9.2对23.5±11.6个PS/秒,P<0.01)。自相关显示,与其他具有近乎周期性行为的区域相比,不规则行为在空间上局限于解剖学异质性。简单的空间PS分布是复杂多变的激活模式的基础,这归因于PS行为、寿命和PS间相互作用的变化。

结论

PSs以非随机的空间分布出现,并与正常解剖学异质性共定位。PS行为和寿命各不相同,但PS空间分布稳定,导致不断变化的激活模式,这是VF的特征。

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