主动脉-腔静脉瘘大鼠肥厚心肌中内皮素-1及内皮素A受体亚型的选择性增加。

Selective increase in endothelin-1 and endothelin A receptor subtype in the hypertrophied myocardium of the aorto-venacaval fistula rat.

作者信息

Brown L A, Nunez D J, Brookes C I, Wilkins M R

机构信息

Department of Clinical Pharmacology, Royal Postgraduate Medical School, Hammersmith Hospital, London, United Kingdom.

出版信息

Cardiovasc Res. 1995 Jun;29(6):768-74.

PMID:7656280

Abstract

OBJECTIVE

At present little is known about the factors that regulate the expression of the endothelins and their receptors in cardiac tissue in vivo. The aim of this study was to investigate changes in expression of the endothelins (ET-1, ET-2, and ET-3) and their receptors (ETAR and ETBR) in the hypertrophied heart of the aortovenocaval (AV) fistula rat.

METHODS

Reverse transcription-polymerase chain reaction (RT-PCR) was used to quantify cardiac mRNA expression of the endothelins and their receptors during the development of cardiac hypertrophy, while radioligand binding was employed to quantify the amount of [125I]-ET-1 binding to cardiac membranes. Tissue and plasma concentrations of ET-1 were measured by radioimmunoassay.

RESULTS

In control sham operated animals, ET-1 mRNA was approximately fivefold greater in atria than in ventricles (P < 0.05), but there were no atrioventricular differences in ET-2 or ET-3 mRNA. In the AV fistula rats there was a prompt three- to fourfold increase in ET-1 mRNA in atria and a progressive five- to sevenfold rise in ventricles during cardiac hypertrophy. There were no changes in ET-2 or ET-3 transcript prevalences, except for a late rise (35 d) in ET-2 mRNA levels in left ventricle. Consistent with ET-1 mRNA measurements, immunoreactive endothelin levels were increased by 7 d in atria, but not in ventricles. In control rat hearts, ETAR mRNA levels were similar in atria and ventricles, but the prevalence of ETBR was approximately sevenfold greater in the former. ETAR mRNA prevalence increased with hypertrophy in all chambers, while ETBR transcript levels were raised only in the right ventricle. There was no significant difference in [125I]-ET-1 binding between atrial samples from 35 d control and 35 d AV fistula rats, suggesting rapid turnover of endothelin receptors balanced by increased transcription from the ETAR gene.

CONCLUSIONS

During cardiac hypertrophy in AV fistula rats there is increased activity of the endothelin system mediated principally by ET-1 and the ETAR subtype.

摘要

目的

目前对于体内心脏组织中调节内皮素及其受体表达的因素知之甚少。本研究旨在探讨主动脉腔静脉（AV）瘘大鼠肥厚心脏中内皮素（ET-1、ET-2和ET-3）及其受体（ETAR和ETBR）的表达变化。

方法

采用逆转录聚合酶链反应（RT-PCR）定量心脏肥大发展过程中内皮素及其受体的心脏mRNA表达，同时采用放射性配体结合法定量[125I]-ET-1与心脏膜的结合量。通过放射免疫分析法测定组织和血浆中ET-1的浓度。

结果

在对照假手术动物中，ET-1 mRNA在心房中的含量比心室中大约高五倍（P < 0.05），但ET-2或ET-3 mRNA在心房和心室之间没有差异。在AV瘘大鼠中，心脏肥大期间心房中ET-1 mRNA迅速增加三到四倍，心室中逐渐增加五到七倍。ET-2或ET-3转录本水平没有变化，除了左心室中ET-2 mRNA水平在后期（35天）有所升高。与ET-1 mRNA测量结果一致，心房中免疫反应性内皮素水平在7天时升高，但心室中没有升高。在对照大鼠心脏中，ETAR mRNA水平在心房和心室中相似，但ETBR在心房中的含量大约高七倍。随着肥大的发展，所有腔室中的ETAR mRNA含量均增加，而ETBR转录本水平仅在右心室中升高。35天对照大鼠和35天AV瘘大鼠心房样本之间的[125I]-ET-1结合没有显著差异，这表明内皮素受体的快速周转通过ETAR基因转录增加而得到平衡。