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人类心房颤动期间连接蛋白与心房激活之间的关系。

Relationship between connexins and atrial activation during human atrial fibrillation.

作者信息

Kanagaratnam Prapa, Cherian Ashok, Stanbridge Rex D L, Glenville Brian, Severs Nicholas J, Peters Nicholas S

机构信息

Heart and Lung Division of Imperial College School of Medicine, and St. Mary's Hospital, London, United Kingdom.

出版信息

J Cardiovasc Electrophysiol. 2004 Feb;15(2):206-16. doi: 10.1046/j.1540-8167.2004.03280.x.

Abstract

INTRODUCTION

Gap junctional connexin proteins (connexin40 [Cx40], connexin43 [Cx43]) are a determinant of myocardial conduction and are implicated in the development of atrial fibrillation (AF). We hypothesized that atrial activation pattern during AF is related to connexin expression and that this relationship is altered by AF-induced remodeling in the fibrillating atria of chronic AF.

METHODS AND RESULTS

Isochronal activation mapping was performed during cardiac surgery on the right atria of patients in chronic AF (n = 13) using an epicardial electrode array. The atrial activation pattern was categorized using a complexity score based on the number of propagating wavefronts of activation and by grouping atria into those capable of uniform planar activation (simple) and those that were not (complex). The activation pattern was correlated with the levels of Cx43 and Cx40 signal measured by immunoconfocal quantification of biopsies from the mapped region. We studied the impact of electrical remodeling by comparing these findings with the unremodeled atria of patients in sinus rhythm during pacing-induced sustained AF (n = 17). In chronic AF, atria with complex activation had lower Cx40 signal than atria showing simple activation (0.013 +/- 0.006 microm(2)/microm(2) vs 0.027 +/- 0.009 microm(2)/microm(2), P < 0.02), with the relative connexin signal (Cx40/Cx40+Cx43) correlating with complexity score (P = 0.01, r =-0.74). This relationship did not occur in the unremodeled atria, and increased heterogeneity of distribution of Cx40 labeling in chronic AF was the only evidence of connexin remodeling that we detected in the overall group.

CONCLUSION

The pattern of atrial activation is related to immunoconfocal connexin signal only in the fully remodeled atria of chronic AF. This suggests that intercellular coupling and pattern of atrial activation are interrelated, but only in conjunction with the remodeling of atrial electrophysiology that occurs in chronic AF.

摘要

引言

缝隙连接蛋白(连接蛋白40 [Cx40]、连接蛋白43 [Cx43])是心肌传导的决定因素,与心房颤动(AF)的发生有关。我们假设AF期间的心房激活模式与连接蛋白表达有关,并且这种关系在慢性AF颤动心房中因AF诱导的重塑而改变。

方法与结果

在心脏手术期间,使用心外膜电极阵列对慢性AF患者(n = 13)的右心房进行等时激活标测。根据激活的传播波前数量,通过将心房分为能够进行均匀平面激活的心房(简单型)和不能进行均匀平面激活的心房(复杂型),使用复杂性评分对心房激活模式进行分类。激活模式与通过对标测区域活检进行免疫共聚焦定量测量的Cx43和Cx40信号水平相关。通过将这些结果与起搏诱导的持续性AF期间窦性心律患者的未重塑心房(n = 17)进行比较,我们研究了电重塑的影响。在慢性AF中,具有复杂激活的心房的Cx40信号低于显示简单激活的心房(0.013±0.006μm²/μm²对0.027±0.009μm²/μm²,P<0.02),连接蛋白相对信号(Cx40/Cx40 + Cx43)与复杂性评分相关(P = 0.01,r = -0.74)。这种关系在未重塑的心房中未出现,并且慢性AF中Cx40标记分布的异质性增加是我们在整个组中检测到的连接蛋白重塑的唯一证据。

结论

心房激活模式仅在慢性AF的完全重塑心房中与免疫共聚焦连接蛋白信号相关。这表明细胞间偶联和心房激活模式是相互关联的,但仅与慢性AF中发生的心房电生理重塑相关。

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