Lawson D, Frazer M J, Lynch C
Department of Anesthesiology, University of Virginia Health Sciences Center, Charlottesville 22908.
Anesthesiology. 1990 Nov;73(5):930-43. doi: 10.1097/00000542-199011000-00022.
This study examined in vitro myocardial depression by 50% N2O. Maximal isometric contractions of guinea pig right ventricular papillary muscles were studied in Tyrode's superfusate at 37 degrees C within a gas-tight chamber. Superfusate (pH at 7.45) and chamber were equilibrated with 95% O2/5% CO2. After control measurements in 95% O2, muscles were studied with 50% N2 and 50% N2O (45% O2/5% CO2) in random order with an intervening and final recovery in oxygen. Muscles were field stimulated after rest and at 0.1-3 Hz. At 37 degrees C, muscle performance deteriorated over time with exposure to reduced oxygen; therefore, identical experiments were performed at 30 degrees C in which no systematic deterioration occurred. Peak tension and maximum rate of tension development (dT/dtmax) were compared for each stimulation rate. At both temperatures, N2O caused a 10-15% depression of contractility as compared to that observed with nitrogen. In a second protocol, muscles were studied at 37 degrees C in 26 mM K+ Tyrode's solution with 0.10 microM isoproterenol to study enhanced contractions mediated by slow (Ca2(+)-channel-dependent) action potentials. Rested-state double stimulations were used (stimulus interval, 250-600 ms) resulting in a first rested-state contraction followed by a second contraction (C2) with rapid initial tension development. The muscles were exposed to nitrogen and N2O as in the force-frequency experiments and did not deteriorate over time. In this setting, N2O also caused a 10-15% depression of C2 contractility as compared with nitrogen. Another set of muscles was studied in 95% O2 to which 0.5% halothane or 1% isoflurane was added before exposure to nitrogen and N2O. The combined depressant action of N2O with either halothane or isoflurane did not differ from that predicted by the simple addition of independent effects; there was no evidence of synergism. Furthermore, N2O (50%) alone depressed dT/dtmax in a manner similar to that of 0.5% halothane and different from that of 1.0% isoflurane. Experiments conducted in iso-osmolar 40 mM Na+ Tyrode's solution, in which activator Ca2+ arose from the sarcoplasmic reticulum Ca2+, also showed greater depression by N2O than nitrogen. N2O (50%) is a myocardial depressant independent of concurrent hypoxic effects with a pattern and magnitude of contractile depression similar to that of 0.5% halothane.
本研究检测了50%氧化亚氮对心肌的体外抑制作用。在37℃的气密小室内,于台氏液中研究豚鼠右心室乳头肌的最大等长收缩。台氏液(pH为7.45)和小室用95%氧气/5%二氧化碳平衡。在95%氧气环境下进行对照测量后,肌肉先后随机暴露于50%氮气和50%氧化亚氮(45%氧气/5%二氧化碳)环境中,中间及最后恢复至氧气环境。肌肉在休息后及0.1 - 3Hz频率下进行场刺激。在37℃时,随着暴露于低氧环境,肌肉性能随时间恶化;因此,在30℃进行了相同实验,在此温度下未出现系统性恶化。比较了每种刺激频率下的峰值张力和最大张力发展速率(dT/dtmax)。在两个温度下,与氮气相比,氧化亚氮均导致收缩力降低10 - 15%。在第二个实验方案中,在含有0.10微摩尔异丙肾上腺素的26毫摩尔钾离子台氏液中于37℃研究肌肉,以探讨由缓慢(钙通道依赖性)动作电位介导的增强收缩。采用静息状态双刺激(刺激间隔250 - 600毫秒),产生第一次静息状态收缩,随后是第二次收缩(C2),其初始张力快速发展。肌肉如在力 - 频率实验中那样暴露于氮气和氧化亚氮环境,且未随时间恶化。在此情况下,与氮气相比,氧化亚氮也使C2收缩力降低10 - 15%。另一组肌肉在95%氧气环境中进行研究,在暴露于氮气和氧化亚氮之前加入0.5%氟烷或1%异氟烷。氧化亚氮与氟烷或异氟烷的联合抑制作用与独立效应简单相加所预测的结果无差异;没有协同作用的证据。此外,单独的50%氧化亚氮降低dT/dtmax的方式类似于0.5%氟烷,不同于1.0%异氟烷。在等渗的40毫摩尔钠离子台氏液中进行的实验,其中激活钙来自肌浆网钙,也显示氧化亚氮比氮气产生更大的抑制作用。50%氧化亚氮是一种心肌抑制剂,与同时存在的低氧效应无关,其收缩抑制的模式和程度类似于0.5%氟烷。
