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犬心室标本中不同钾通道在心脏复极化过程中的相互作用:复极化储备的作用

Interaction of different potassium channels in cardiac repolarization in dog ventricular preparations: role of repolarization reserve.

作者信息

Biliczki Péter, Virág László, Iost Norbert, Papp Julius Gy, Varró András

机构信息

Department of Pharmacology & Pharmacotherapy, Faculty of Medicine, University of Szeged, Szeged, Hungary.

出版信息

Br J Pharmacol. 2002 Oct;137(3):361-8. doi: 10.1038/sj.bjp.0704881.

Abstract

1 The aim of this study was to investigate the possible role of the interaction of different potassium channels in dog ventricular muscle, by applying the conventional microelectrode and whole cell patch-clamp techniques at 37 degrees C. 2 Complete block of I(Kr) by 1 micro M dofetilide lengthened action potential duration (APD) by 45.6+/-3.6% at 0.2 Hz (n=13). Chromanol 293B applied alone at 10 micro M (a concentration which selectively blocks I(Ks)) did not markedly lengthen APD (<7%), but when repolarization had already been prolonged by complete I(Kr) block with 1 micro M dofetilide, inhibition of I(Ks) with 10 micro M chromanol 293B substantially delayed repolarization by 38.5+/-8.2% at 0.2 Hz (n=6). 3 BaCl(2), at a concentration of 10 micro M which blocks I(Kl) without affecting other currents, lengthened APD by 33.0+/-3.1% (n=11), but when I(Kr) was blocked with 1 micro M dofetilide, 10 micro M BaCl(2) produced a more excessive rate dependent lengthening in APD, frequently (in three out of seven preparations) initiating early afterdepolarizations. 4 These findings indicate that if only one type of potassium channels is inhibited in dog ventricular muscle, excessive APD lengthening is not likely to occur. Dog ventricular myocytes seem to repolarize with a strong safety margin ('repolarization reserve'). However, when this normal 'repolarization reserve' is attenuated, otherwise minimal or moderate potassium current inhibition can result in excessive and potentially proarrhythmic prolongation of the ventricular APD. Therefore, application of drugs which are able to block more than one type of potassium channel is probably more hazardous than the use of a specific inhibitor of one given sort of potassium channel, and when simultaneous blockade of several kinds of potassium channel may be presumed, a detailed study is needed to define the determinants of 'repolarization reserve'.

摘要
  1. 本研究的目的是通过在37℃下应用传统微电极和全细胞膜片钳技术,研究犬心室肌中不同钾通道相互作用的可能作用。2. 1 μM多非利特对I(Kr)的完全阻断使0.2 Hz时动作电位时程(APD)延长了45.6±3.6%(n = 13)。单独应用10 μM的色满醇293B(一种选择性阻断I(Ks)的浓度)并未显著延长APD(<7%),但当用1 μM多非利特完全阻断I(Kr)已使复极化延长时,用10 μM色满醇293B抑制I(Ks)在0.2 Hz时使复极化显著延迟了38.5±8.2%(n = 6)。3. 浓度为10 μM的BaCl₂可阻断I(Kl)而不影响其他电流,使APD延长了33.0±3.1%(n = 11),但当用1 μM多非利特阻断I(Kr)时,10 μM BaCl₂使APD产生更明显的频率依赖性延长,经常(在7个标本中有3个)引发早期后去极化。4. 这些发现表明,如果犬心室肌中仅一种类型的钾通道受到抑制,不太可能发生过度的APD延长。犬心室肌细胞似乎以很强的安全边际(“复极化储备”)进行复极化。然而,当这种正常的“复极化储备”减弱时,否则最小或中度的钾电流抑制可导致心室APD过度延长并可能引发心律失常。因此,应用能够阻断不止一种类型钾通道的药物可能比使用一种特定类型钾通道的特异性抑制剂更具危险性,并且当可能推测几种钾通道同时被阻断时,需要进行详细研究以确定“复极化储备”的决定因素。

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