Baumgart D, Ehring T, Krajcar M, Skyschally A, Heusch G
Department of Pathophysiology, University of Essen Medical School, FRG.
Basic Res Cardiol. 1994 Jan-Feb;89(1):61-79. doi: 10.1007/BF00788678.
Positive inotropic substances which enhance the myocardial cAMP level or inhibit the Na+/K(+)-ATPase are known for their proarrhythmic side-effects. This study was performed to investigate the inotropic and arrhythmogenic action of the Na(+)-channel activator BDF 9148 (racemate) in comparison to its S-enantiomer BDF 9196, its congener DPI 201-106 (racemate), to norepinephrine, and to ouabain. In 30 open-chest dogs, the effects of these substances on the first derivative of left ventricular pressure (dP/dt, Millar-tip catheter) and anterior systolic wall thickening (AWT, sonomicrometry) were studied. Concomitantly, myocardial excitability, conduction times, and refractory period were assessed with a transmural, three-dimensional, 16-electrode array in the anterior wall. For the study of the Na(+)-channel activators, alpha- and beta-adrenergic and muscarinic receptors were blocked. A first set of measurements was performed during normoperfusion with administration of BDF 9148 (1 mg/kg, n = 8), BDF 9196 (0.5 mg/kg, n = 8), and DPI 201-106 (1 mg/kg, n = 8), respectively. A second set of measurements was performed with administration of the threefold dosage of either substance. With a severe stenosis on the left anterior descending coronary artery, a final set of measurements was performed, again using the higher dosage of either substance. For the study of norepinephrine (0.5 micrograms/kg/min i.v., n = 6) and ouabain (40 micrograms/kg i.v., n = 4), measurements were performed during normoperfusion in additional animals. Under normal conditions, either Na(+)-channel activator induced increases in dP/dtmax (lower dosage: 45-84%, higher dosage: by 93-117%) and AWT (lower dosage: by 24-37%, higher dosage: by 19-56%). Under ischemic conditions, either drug increased dP/dtmax by 60-98% and AWT by 45-102%. Excitability, conduction times, and refractory period did not change significantly in response to the Na(+)-channel activators, neither under normal nor under ischemic conditions. There was no significant difference in the incidence of spontaneous ventricular extrasystoles before and after administration of either Na(+)-channel activator. In contrast, an equi-inotropic dosage of norepinephrine (increases in dP/dtmax by 148% and AWT by 42%) increased excitability, decreased conduction times and refractory period, and increased the incidence of spontaneous ventricular extrasystoles. Ouabain induced only a moderate increase in dP/dtmax by 56% and AWT by 24%, but elicited sustained and complex ventricular arrhythmias. Excitability was markedly increased, whereas conduction times and refractory period changed only little.(ABSTRACT TRUNCATED AT 400 WORDS)
增强心肌环磷酸腺苷(cAMP)水平或抑制钠钾ATP酶的正性肌力物质,以其致心律失常的副作用而闻名。本研究旨在比较钠通道激活剂BDF 9148(消旋体)与其S-对映体BDF 9196、同类物DPI 201-106(消旋体)、去甲肾上腺素和哇巴因的正性肌力作用和致心律失常作用。在30只开胸犬中,研究了这些物质对左心室压力一阶导数(dP/dt,Millar尖端导管)和收缩期前壁增厚(AWT,超声心动图)的影响。同时,使用前壁的透壁三维16电极阵列评估心肌兴奋性、传导时间和不应期。为研究钠通道激活剂,α和β肾上腺素能受体及毒蕈碱受体被阻断。第一组测量在正常灌注期间进行,分别给予BDF 9148(1 mg/kg,n = 8)、BDF 9196(0.5 mg/kg,n = 8)和DPI 201-106(1 mg/kg,n = 8)。第二组测量给予每种物质三倍剂量后进行。在左前降支冠状动脉严重狭窄的情况下,再次使用每种物质的较高剂量进行最后一组测量。为研究去甲肾上腺素(0.5微克/千克/分钟静脉注射,n = 6)和哇巴因(40微克/千克静脉注射,n = 4),在另外的动物正常灌注期间进行测量。在正常条件下,两种钠通道激活剂均可使dP/dtmax增加(低剂量:45 - 84%,高剂量:93 - 117%)和AWT增加(低剂量:24 - 37%,高剂量:19 - 56%)。在缺血条件下,两种药物均可使dP/dtmax增加60 - 98%,使AWT增加45 - 102%。钠通道激活剂对兴奋性、传导时间和不应期无显著影响,无论是在正常还是缺血条件下。给予任何一种钠通道激活剂前后,自发性室性早搏的发生率均无显著差异。相比之下,等正性肌力剂量的去甲肾上腺素(dP/dtmax增加148%,AWT增加42%)可增加兴奋性、缩短传导时间和不应期,并增加自发性室性早搏的发生率。哇巴因仅使dP/dtmax适度增加56%,使AWT增加24%,但引发持续性和复杂性室性心律失常。兴奋性明显增加,而传导时间和不应期变化很小。(摘要截短至400字)
