REENTRANT TACHYCARDIA IN A THIN-LAYER OF VENTRICULAR SUBEPICARDIUM - EFFECTS OF D-SOTALOL AND LIDOCAINE

被引：19

作者：

HILL, BC ^{[1
]}

HUNT, AJ ^{[1
]}

COURTNEY, KR ^{[1
]}

机构：

[1] PALO ALTO MED RES FDN, RES INST, DEPT CARDIOVASC PHYSIOL & BIOPHYS, 860 BRYANT ST, PALO ALTO, CA 94301 USA

来源：

JOURNAL OF CARDIOVASCULAR PHARMACOLOGY | 1990年 / 16卷 / 06期

关键词：

Anisotropy; Class I antiarrhythmics; Proarrhythmia; Reentry; Ventricular tachycardia; Wavelength;

D O I：

10.1097/00005344-199012000-00003

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Ventricular tachycardia (VT) was induced by premature stimulation or fast pacing in 14 Langendorff-perfused rabbit hearts whose left ventricular endocardial and intramural cells had been selectively killed by freezing. VTs were caused by apparent reentrant excitation in the surviving thin (1 mm thick) subepicardial layer of anisotropically oriented cells having ostensibly normal membrane characteristics. During VT, 100 μM d-sotalol (seven hearts) or 30 μM lidocaine (seven hearts) was added to the perfusate. Electrophysiological variables were measured before and during drug exposure at both slow (S1 = 300 ms) and fast (S1 = 150-180 ms) pacing rates. Sotalol prevented VT reinduction in six of seven preparations, compared to only two of seven with lidocaine. Lidocaine prolonged the functional refractory period (FRP) and slowed conduction velocity (CV). Lidocaine prolonged the wavelength of the cardiac impulse (=FRP × CV) by 18% at slow rates but reduced it by 21% at fast rates. Sotalol, however, since it increased the FRP without reducing CV, caused wavelength prolongation at both rates (43% at slow rates, 26% at fast rates). Thus, this VT model may provide an important contrast of class I and class III drug action, with the drug effects on wavelength predicting susceptibility to VT induction. © 1990 Raven Press, Ltd., New York.

引用

页码：871 / 880

页数：10

共 61 条

[1] CIRCUS MOVEMENT IN RABBIT ATRIAL MUSCLE AS A MECHANISM OF TACHYCARDIA .2. ROLE OF NONUNIFORM RECOVERY OF EXCITABILITY IN OCCURRENCE OF UNIDIRECTIONAL BLOCK, AS STUDIED WITH MULTIPLE MICROELECTRODES [J].

ALLESSIE, MA ;

BONKE, FIM ;

SCHOPMAN, FJG .

CIRCULATION RESEARCH, 1976, 39 (02) :168-177

[2] CIRCUS MOVEMENT IN RABBIT ATRIAL MUSCLE AS A MECHANISM OF TACHYCARDIA .3. LEADING CIRCLE CONCEPT - NEW MODEL OF CIRCUS MOVEMENT IN CARDIAC TISSUE WITHOUT INVOLVEMENT OF AN ANATOMICAL OBSTACLE [J].

ALLESSIE, MA ;

BONKE, FIM ;

SCHOPMAN, FJG .

CIRCULATION RESEARCH, 1977, 41 (01) :9-18

[3] EXPERIMENTAL ELECTROPHYSIOLOGY AND ARRHYTHMOGENICITY - ANISOTROPY AND VENTRICULAR-TACHYCARDIA [J].

ALLESSIE, MA ;

SCHALIJ, MJ ;

KIRCHHOF, CJHJ ;

BOERSMA, L ;

HUYBERS, M ;

HOLLEN, J .

EUROPEAN HEART JOURNAL, 1989, 10 :2-8

[4]

ALLESSIE MA, 1988, CIRCULATION S2, V78, P612

[5] THE EFFECTS OF ANTIARRHYTHMIC DRUGS, STIMULATION FREQUENCY, AND POTASSIUM-INDUCED RESTING MEMBRANE-POTENTIAL CHANGES ON CONDUCTION-VELOCITY AND DV/DTMAX IN GUINEA-PIG MYOCARDIUM [J].

BUCHANAN, JW ;

SAITO, T ;

GETTES, LS .

CIRCULATION RESEARCH, 1985, 56 (05) :696-703

[6] CELLULAR ELECTROPHYSIOLOGICAL EFFECTS OF D-SOTALOL AND DL-SOTALOL IN GUINEA-PIG SINOATRIAL NODE, ATRIUM AND VENTRICLE AND HUMAN ATRIUM - DIFFERENTIAL TISSUE SENSITIVITY [J].

CAMPBELL, TJ .

BRITISH JOURNAL OF PHARMACOLOGY, 1987, 90 (03) :593-599

[7] ANISOTROPIC CONDUCTION AND FUNCTIONAL DISSOCIATION OF ISCHEMIC TISSUE DURING REENTRANT VENTRICULAR-TACHYCARDIA IN CANINE MYOCARDIAL-INFARCTION [J].

CARDINAL, R ;

VERMEULEN, M ;

SHENASA, M ;

ROBERGE, F ;

PAGE, P ;

HELIE, F ;

SAVARD, P .

CIRCULATION, 1988, 77 (05) :1162-1176

[8]

CARMELIET E, 1985, J PHARMACOL EXP THER, V232, P817

[9] ACTION OF SOTALOL ON POTENTIAL REENTRANT PATHWAYS AND VENTRICULAR TACHYARRHYTHMIAS IN CONSCIOUS DOGS IN THE LATE POSTMYOCARDIAL INFARCTION PHASE [J].

COBBE, SM ;

HOFFMAN, E ;

RITZENHOFF, A ;

BRACHMANN, J ;

KUBLER, W ;

SENGES, J .

CIRCULATION, 1983, 68 (04) :865-871

[10]

COOPER MJ, 1989, CIRCULATION, V80, P326

← 1 2 3 4 5 6 7 →