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心血管系统中的钾通道。

Potassium channels in the cardiovascular system.

作者信息

Pogátsa G

机构信息

National Institute of Cardiology, Research Department, Budapest, Hungary.

出版信息

Diabetes Res Clin Pract. 1995 Aug;28 Suppl:S91-8. doi: 10.1016/0168-8227(95)01103-k.

DOI:10.1016/0168-8227(95)01103-k
PMID:8529523
Abstract

In vitro and in vivo studies suggest that opening of ATP-sensitive potassium channels following ischaemia enhances recovery of myocardial contraction, dilates blood vessels and has an antiarrhythmic effect. Different sulphonylurea compounds that block the ATP-sensitive potassium channels exert different effects on cardiac functions. Glibenclamide decrease, arrhythmogenesis during acute myocardial infarction in rats and reduces strophanthin cardiotoxicity in rabbits. Other sulphonylurea compounds, but not glibenclamide, increase arterial blood pressure and myocardial contractility. These effects may be partly secondary to blockade of ATP-sensitive potassium channels and partly due to independent cardiac and extracardiac actions. Glimepiride may have a more advantageous cardiovascular effect than glibenclamide. The studies suggest the hypothesis that deleterious cardiovascular effects of some hypoglycaemic sulphonylurea drugs may contribute to the high cardiovascular mortality rate in diabetes mellitus. An observational study suggested glibenclamide decreased the incidence of fatal myocardial infarction and development of ventricular fibrillation in patients suffering from acute myocardial infarction. Glibenclamide may also decrease the incidence of ventricular ectopic beats in digitalized patients compared with other sulphonylurea compounds. The studies suggested the survival of subjects treated with glibenclamide, insulin, or diet alone after the first attack of angina pectoris or after first acute myocardial infarction may be longer compared with those on other sulphonylurea therapies. Further large scale prospective, randomised studies are needed to determine whether the reported effects can be verified and are sufficiently large to affect clinical prescribing.

摘要

体外和体内研究表明,缺血后ATP敏感性钾通道的开放可增强心肌收缩恢复、扩张血管并具有抗心律失常作用。不同的磺酰脲类化合物阻断ATP敏感性钾通道后对心脏功能产生不同影响。格列本脲可降低大鼠急性心肌梗死期间的心律失常发生率,并降低毒毛花苷对家兔的心脏毒性。其他磺酰脲类化合物(而非格列本脲)可升高动脉血压并增强心肌收缩力。这些作用可能部分继发于对ATP敏感性钾通道的阻断,部分归因于独立的心脏和心脏外作用。格列美脲可能比格列本脲具有更有利的心血管效应。这些研究提出了一个假说,即某些降糖磺酰脲类药物的有害心血管效应可能导致糖尿病患者心血管死亡率较高。一项观察性研究表明,格列本脲可降低急性心肌梗死患者致命性心肌梗死的发生率和室颤的发生。与其他磺酰脲类化合物相比,格列本脲还可能降低洋地黄化患者室性早搏的发生率。这些研究表明,与接受其他磺酰脲类治疗的患者相比,在首次心绞痛发作或首次急性心肌梗死后接受格列本脲、胰岛素或单纯饮食治疗的患者存活时间可能更长。需要进一步进行大规模前瞻性随机研究来确定所报道的效应是否能够得到证实,以及其影响临床处方的程度是否足够大。

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1
Potassium channels in the cardiovascular system.心血管系统中的钾通道。
Diabetes Res Clin Pract. 1995 Aug;28 Suppl:S91-8. doi: 10.1016/0168-8227(95)01103-k.
2
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