α1A-和α1B-肾上腺素能受体亚型均与大鼠心室肌细胞的瞬时外向电流（I(To)）相关联。

Both alpha(1A)- and alpha(1B)-adrenergic receptor subtypes couple to the transient outward current (I(To)) in rat ventricular myocytes.

作者信息

Homma N, Hirasawa A, Shibata K, Hashimito K, Tsujimoto G

机构信息

Department of Pharmacology, Yamanashi Medical College, Shimokatoh-1110, Tamaho-Cho, Yamanashi, 409-38 Japan.

出版信息

Br J Pharmacol. 2000 Mar;129(6):1113-20. doi: 10.1038/sj.bjp.0703179.

DOI:10.1038/sj.bjp.0703179

PMID:10725259

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1571955/

Abstract

Regulation of transient outward current (I(To)) by alpha(1)-adrenergic (alpha(1)AR) plays a key role in cardiac repolarization. alpha(1)ARs comprise a heterogeneous family; two natively expressed subtypes (alpha(1A) and alpha(1B)) and three cloned subtypes (alpha(1a), alpha(1b) and alpha(1d)) can be distinguished. We have examined the electrophysiological role of each alpha(1)AR subtype in regulating I(To) in isolated rat ventricular myocytes. 2. Reverse transcription-PCR study revealed the presence of three subtype mRNAs (alpha(1a), alpha(1b) and alpha(1d)) in rat myocytes. 3. Radioligand binding assay using [(125)I]-HEAT showed that the inhibition curves for alpha(1A)AR-selective antagonists (WB4101, 5-methylurapidil, (+)-niguldipine and KMD-3213) in rat ventricles best fit a two-site model, with 30% high and 70% low affinity binding sites. The high affinity sites were resistant to 100 microM chloroethylclonidine (CEC), while the low affinity sites were highly inactivated by CEC. 4. Whole cell voltage clamp study revealed that methoxamine reduced a 4-aminopyridine(4-AP)-sensitive component of I(To) in the isolated rat ventricle myocytes. Lower concentrations of KMD-3213 (1 nM) or 5-MU (10 nM) did not affect the methoxamine-induced reduction of I(To). On the other hand, CEC treatment (100 microM) of isolated myocytes reduced the methoxamine-induced reduction of I(To) by 46%, and the remaining response was abolished by lower concentrations of KMD-3213 or 5-MU. 5. The results indicate that rat ventricular myocytes express transcripts of the three alpha(1)AR subtypes (alpha(1a), alpha(1b) and alpha(1d)); however, two pharmacologically distinct alpha(1)AR subtypes (alpha(1A) and alpha(1B)) are predominating in receptor populations, with approximately 30% alpha(1A)AR and 70% alpha(1B)AR. Although both alpha(1A) and alpha(1B)AR subtypes are coupled to the cardiac I(To), alpha(1B)ARs predominantly mediate alpha(1)AR-induced effect.

摘要

α1 - 肾上腺素能受体（α1AR）对瞬时外向电流（I(To)）的调节在心脏复极化过程中起关键作用。α1ARs是一个异质性家族；可区分出两种天然表达的亚型（α1A和α1B）以及三种克隆亚型（α1a、α1b和α1d）。我们研究了每种α1AR亚型在调节分离的大鼠心室肌细胞I(To)中的电生理作用。2. 逆转录 - PCR研究显示大鼠心肌细胞中存在三种亚型的mRNA（α1a、α1b和α1d）。3. 使用[(125)I]-HEAT的放射性配体结合试验表明，α1A受体选择性拮抗剂（WB4101、5 - 甲基乌拉地尔、(+) - 尼莫地平及KMD - 3213）对大鼠心室的抑制曲线最符合双位点模型，其中高亲和力结合位点占30%，低亲和力结合位点占70%。高亲和力位点对100μM氯乙可乐定（CEC）有抗性，而低亲和力位点被CEC高度灭活。4. 全细胞电压钳研究表明，甲氧明降低了分离的大鼠心室肌细胞中4 - 氨基吡啶（4 - AP）敏感的I(To)成分。较低浓度的KMD - 3213（1 nM）或5 - MU（10 nM）不影响甲氧明诱导的I(To)降低。另一方面，用CEC（100μM）处理分离的心肌细胞可使甲氧明诱导的I(To)降低减少46%，而剩余的反应可被较低浓度的KMD - 3213或5 - MU消除。5. 结果表明，大鼠心室肌细胞表达三种α1AR亚型（α1a、α1b和α1d）的转录本；然而，在受体群体中两种药理学上不同的α1AR亚型（α1A和α1B）占主导，其中α1A受体约占30%，α1B受体约占70%。尽管α1A和α1B受体亚型均与心脏I(To)偶联，但α1B受体主要介导α1AR诱导的效应。