QUINIDINE-INDUCED OPEN-CHANNEL BLOCK OF K+ CURRENT IN RAT VENTRICLE

被引：50

作者：

CLARK, RB ^{[1
]}

SANCHEZCHAPULA, J ^{[1
]}

SALINASSTEFANON, E ^{[1
]}

DUFF, HJ ^{[1
]}

GILES, WR ^{[1
]}

机构：

[1] UNIV CALGARY,SCH MED,DEPT MED,CALGARY,AB T2N 4N1,CANADA

来源：

BRITISH JOURNAL OF PHARMACOLOGY | 1995年 / 115卷 / 02期

关键词：

VOLTAGE-CLAMP; K+ CURRENT; ANTIARRHYTHMIC DRUGS; REPOLARIZATION;

D O I：

10.1111/j.1476-5381.1995.tb15882.x

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

1 The effects of quinidine on calcium-independent outward K+ currents in rat ventricular myocytes were studied using whole-cell patch clamp techniques. 2 Quinidine sulphate (6 mu M) significantly prolonged repolarization of the ventricular action potential. This effect was larger during early repolarization (25% level) than at later times (90% level). 3 Quinidine reduced the amplitude of a transient outward current, and accelerated its rate of decay by approximately 4 fold at membrane potentials between 0 to +50 mV. Quinidine also reduced the amplitude of a slowly inactivating, tetraethylammonium-sensitive 'pedestal' component of the outward current. 4 The quinidine-induced block of the transient outward current was dependent on time and membrane potential. Maximal block occurred with depolarizations of about 100 ms duration, and longer depolarizations (up to 1.5 s) produced little additional block. The membrane potential dependence of quinidine-induced block was very similar to the membrane potential dependence of activation of the transient outward current. The membrane potential dependence of steady-state inactivation of the transient outward current was not significantly affected by quinidine. 5 These results show that quinidine blocks outward K+ currents in rat ventricular cells. The time and potential dependence of this block suggests that quinidine blocks the transient outward K+ current by acting primarily on the open state of these channels.

引用

页码：335 / 343

页数：9

共 41 条

[1] CHARACTERIZATION OF 2 DISTINCT DEPOLARIZATION-ACTIVATED K+ CURRENTS IN ISOLATED ADULT-RAT VENTRICULAR MYOCYTES [J].

APKON, M ;

NERBONNE, JM .

JOURNAL OF GENERAL PHYSIOLOGY, 1991, 97 (05) :973-1011

[2] INTERACTION OF TETRAETHYLAMMONIUM ION DERIVATIVES WITH POTASSIUM CHANNELS OF GIANT AXONS [J].

ARMSTRONG, CM .

JOURNAL OF GENERAL PHYSIOLOGY, 1971, 58 (04) :413-+

[3] SINGLE INWARD RECTIFIER POTASSIUM CHANNELS IN GUINEA-PIG VENTRICULAR MYOCYTES - EFFECTS OF QUINIDINE [J].

BALSER, JR ;

RODEN, DM ;

BENNETT, PB .

BIOPHYSICAL JOURNAL, 1991, 59 (01) :150-161

[4] SUPPRESSION OF TIME-DEPENDENT OUTWARD CURRENT IN GUINEA-PIG VENTRICULAR MYOCYTES - ACTIONS OF QUINIDINE AND AMIODARONE [J].

BALSER, JR ;

BENNETT, PB ;

HONDEGHEM, LM ;

RODEN, DM .

CIRCULATION RESEARCH, 1991, 69 (02) :519-529

[5]

BAUMGARTEN CM, 1991, HEART CARDIOVASCULAR, P963

[6] HETEROGENEITY OF ACTION-POTENTIAL WAVE-FORMS AND POTASSIUM CURRENTS IN RAT VENTRICLE [J].

CLARK, RB ;

BOUCHARD, RA ;

SALINASSTEFANON, E ;

SANCHEZCHAPULA, J ;

GILES, WR .

CARDIOVASCULAR RESEARCH, 1993, 27 (10) :1795-1799

[7] EVIDENCE FOR A SPECIFIC RECEPTOR-SITE FOR LIDOCAINE, QUINIDINE, AND BUPIVACAINE ASSOCIATED WITH CARDIAC SODIUM-CHANNELS IN GUINEA-PIG VENTRICULAR MYOCARDIUM [J].

CLARKSON, CW ;

HONDEGHEM, LM .

CIRCULATION RESEARCH, 1985, 56 (04) :496-506

[8] CHANNEL SPECIFICITY IN ANTIARRHYTHMIC DRUG-ACTION - MECHANISM OF POTASSIUM CHANNEL BLOCK AND ITS ROLE IN SUPPRESSING AND AGGRAVATING CARDIAC-ARRHYTHMIAS [J].

COLATSKY, TJ ;

FOLLMER, CH ;

STARMER, CF .

CIRCULATION, 1990, 82 (06) :2235-2242

[9] MECHANISMS OF ACTION OF LIDOCAINE AND QUINIDINE ON ACTION-POTENTIAL DURATION IN RABBIT CARDIAC PURKINJE-FIBERS - AN EFFECT ON STEADY-STATE SODIUM CURRENTS [J].

COLATSKY, TJ .

CIRCULATION RESEARCH, 1982, 50 (01) :17-27

[10]

FURUKAWA T, 1989, J PHARMACOL EXP THER, V251, P756

← 1 2 3 4 5 →