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人类特化房室传导轴的分子结构。

Molecular architecture of the human specialised atrioventricular conduction axis.

机构信息

Cardiovascular Medicine, Faculty of Medical and Human Sciences, University of Manchester, UK.

出版信息

J Mol Cell Cardiol. 2011 Apr;50(4):642-51. doi: 10.1016/j.yjmcc.2010.12.017. Epub 2011 Jan 21.

DOI:10.1016/j.yjmcc.2010.12.017
PMID:21256850
Abstract

The atrioventricular conduction axis, located in the septal component of the atrioventricular junctions, is arguably the most complex structure in the heart. It fulfils a multitude of functions, including the introduction of a delay between atrial and ventricular systole and backup pacemaking. Like any other multifunctional tissue, complexity is a key feature of this specialised tissue in the heart, and this complexity is both anatomical and electrophysiological, with the two being inextricably linked. We used quantitative PCR, histology and immunohistochemistry to analyse the axis from six human subjects. mRNAs for ~50 ion and gap junction channels, Ca(2+)-handling proteins and markers were measured in the atrial muscle (AM), a transitional area (TA), inferior nodal extension (INE), compact node (CN), penetrating bundle (PB) and ventricular muscle (VM). When compared to the AM, we found a lower expression of Na(v)1.5, K(ir)2.1, Cx43 and ANP mRNAs in the CN for example, but a higher expression of HCN1, HCN4, Ca(v)1.3, Ca(v)3.1, K(ir)3.4, Cx40 and Tbx3 mRNAs. Expression of some related proteins was in agreement with the expression of the corresponding mRNAs. There is a complex and heterogeneous pattern of expression of ion and gap junction channels and Ca(2+)-handling proteins in the human atrioventricular conduction axis that explains the function of this crucial pathway.

摘要

房室传导轴位于房室结的间隔成分中,可以说是心脏中最复杂的结构。它具有多种功能,包括在心房和心室收缩之间引入延迟和备用起搏。像任何其他多功能组织一样,这种心脏特化组织的复杂性是其关键特征,这种复杂性既有解剖学上的,也有电生理学上的,两者紧密相连。我们使用定量 PCR、组织学和免疫组织化学方法分析了来自 6 名人类受试者的轴。在心房肌(AM)、过渡区(TA)、下结延伸部(INE)、致密结部(CN)、穿透束(PB)和心室肌(VM)中测量了~50 种离子和缝隙连接通道、Ca(2+)处理蛋白和标志物的 mRNA。与 AM 相比,例如,我们发现 CN 中的 Na(v)1.5、K(ir)2.1、Cx43 和 ANP mRNA 的表达降低,但 HCN1、HCN4、Ca(v)1.3、Ca(v)3.1、K(ir)3.4、Cx40 和 Tbx3 mRNA 的表达增加。一些相关蛋白的表达与相应的 mRNA 表达一致。人类房室传导轴中离子和缝隙连接通道以及 Ca(2+)处理蛋白的表达具有复杂而异质的模式,解释了这条关键途径的功能。

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