Markel M L, Miles W M, Luck J C, Klein L S, Prystowsky E N
Krannert Institute of Cardiology, Indianapolis, Ind.
Circulation. 1993 Mar;87(3):783-92. doi: 10.1161/01.cir.87.3.783.
Autonomic modulation, especially increased sympathetic activity may play a role in the genesis of ventricular arrhythmias. The purpose of this study was to determine whether beta-sympathetic stimulation with isoproterenol would alter sustained ventricular tachycardia (VT) circuits similarly during the drug-free and antiarrhythmic drug-treated states.
Twenty-five patients with repeatedly inducible, hemodynamically stable, sustained VT were evaluated by programmed ventricular stimulation. In the antiarrhythmic drug-free state, isoproterenol (0.03 microgram/kg per minute) shortened the following intervals (in milliseconds; mean +/- SEM; 25 patients; paired t test): sinus cycle length (792 +/- 37 to 568 +/- 18; (p < 0.001), ventricular paced QT interval (386 +/- 8 to 348 +/- 6; p < 0.001), ventricular paced QRS duration (185 +/- 4 to 182 +/- 4; p = 0.014), ventricular effective (238 +/- 5 to 208 +/- 4; p < 0.001) and functional (261 +/- 6 to 227 +/- 5; p < 0.001) refractory periods, and the VT cycle length (VTCL) (311 +/- 9 to 291 +/- 9; p < 0.001). Isoproterenol (0.03 microgram/kg per minute) was administered during 31 antiarrhythmic drug trials (procainamide, n = 18; quinidine, n = 13) in 22 patients. Isoproterenol shortened the sinus cycle length, QT interval during ventricular pacing, and ventricular effective and functional refractory periods before and during procainamide and quinidine therapy (ANOVA; isoproterenol effect, p < or = 0.0002 for all). The amount of decrease in these intervals with isoproterenol was the same before and during procainamide and quinidine therapy (ANOVA interaction, p = NS for all). The QRS duration during ventricular pacing and VTCL were also shortened by isoproterenol before and during procainamide (baseline, n = 17; QRS, 182 +/- 4 to 178 +/- 4 msec; VTCL, n = 18, 314 +/- 11 to 291 +/- 11 msec; during procainamide, QRS, 218 +/- 7 to 197 +/- 6 msec; VTCL, 422 +/- 15 to 359 +/- 11 msec) and quinidine (baseline, n = 13; QRS, 190 +/- 6 to 185 +/- 5 msec; VTCL, n = 12, 298 +/- 10 to 280 +/- 9 msec; during quinidine, QRS, 223 +/- 9 to 208 +/- 8 msec; VTCL, 415 +/- 14 to 355 +/- 10 msec) (isoproterenol effect p < or = 0.0003 for all). However, the amount of decrease in QRS duration and VTCL with isoproterenol was greater during procainamide and quinidine than in the drug-free state (ANOVA interaction, p < or = 0.02 for all). These changes continued to be significant when normalized for the initial QRS duration and VTCL (p < or = 0.03 for all).
Isoproterenol affects presumed reentrant sustained VT circuits less in the absence of antiarrhythmic drugs but markedly attenuates the antiarrhythmic drug-induced slowing of sustained VT. To the extent that the change in QRS duration reflects a change in conduction within the VT circuit, these data imply that the attenuation of drug-induced slowing of VT by isoproterenol is due to a greater change in conduction rather than refractoriness.
自主神经调节,尤其是交感神经活动增强可能在室性心律失常的发生中起作用。本研究的目的是确定在无抗心律失常药物状态和抗心律失常药物治疗状态下,异丙肾上腺素对β-交感神经的刺激是否会以相似的方式改变持续性室性心动过速(VT)环路。
通过程控心室刺激对25例反复可诱发、血流动力学稳定的持续性VT患者进行评估。在无抗心律失常药物状态下,异丙肾上腺素(0.03微克/千克每分钟)缩短了以下间期(以毫秒计;平均值±标准误;25例患者;配对t检验):窦性周期长度(792±37至568±18;(p<0.001),心室起搏QT间期(386±8至348±6;p<0.001),心室起搏QRS时限(185±4至182±4;p = 0.014),心室有效(238±5至208±4;p<0.001)和功能(261±6至227±5;p<0.001)不应期,以及VT周期长度(VTCL)(311±9至291±9;p<0.001)。在22例患者的31次抗心律失常药物试验(普鲁卡因胺,n = 18;奎尼丁,n = 13)期间给予异丙肾上腺素(0.03微克/千克每分钟)。异丙肾上腺素缩短了在普鲁卡因胺和奎尼丁治疗之前和期间的窦性周期长度、心室起搏期间的QT间期以及心室有效和功能不应期(方差分析;异丙肾上腺素效应,所有p≤0.0002)。在普鲁卡因胺和奎尼丁治疗之前和期间,异丙肾上腺素使这些间期缩短的程度相同(方差分析交互作用,所有p =无显著性差异)。在普鲁卡因胺之前和期间以及奎尼丁治疗期间,心室起搏时的QRS时限和VTCL也被异丙肾上腺素缩短(基线,n = 17;QRS,182±4至178±4毫秒;VTCL,n = 18,314±11至291±11毫秒;在普鲁卡因胺治疗期间,QRS,218±7至197±6毫秒;VTCL,422±15至359±11毫秒)以及奎尼丁(基线,n = 13;QRS,190±6至185±5毫秒;VTCL,n = 12,298±10至280±9毫秒;在奎尼丁治疗期间,QRS,223±9至208±8毫秒;VTCL,415±14至355±10毫秒)(所有异丙肾上腺素效应p≤0.0003)。然而,在普鲁卡因胺和奎尼丁治疗期间,异丙肾上腺素使QRS时限和VTCL缩短的程度大于无药物状态(方差分析交互作用,所有p≤0.02)。当以初始QRS时限和VTCL进行标准化时,这些变化仍然显著(所有p≤0.03)。
在没有抗心律失常药物的情况下,异丙肾上腺素对假定的折返性持续性VT环路的影响较小,但显著减弱了抗心律失常药物引起的持续性VT减慢。就QRS时限的变化反映VT环路内传导的变化而言,这些数据表明异丙肾上腺素减弱药物引起的VT减慢是由于传导的更大变化而非不应期的改变。
