Department of Anesthesiology, Weill Cornell Medical College, New York, New York, USA.
Anesthesiology. 2010 Apr;112(4):892-9. doi: 10.1097/ALN.0b013e3181d32016.
Neuromuscular blocking agents are an integral component of general anesthesia. In addition to their intended pharmacologic target on skeletal muscle nicotinic receptors, undesirable airway effects (i.e., bronchoconstriction) can result from neuromuscular blocking agents' affinity for airway muscarinic receptors. We questioned whether two new members of a bisquaternary nondepolarizing muscle relaxant family, gantacurium and CW002, demonstrated detrimental effects of airway muscarinic receptors using an in vivo model in guinea pig airways.
Urethane-anesthetized male guinea pigs were ventilated through a tracheostomy with continuous digital recordings of pulmonary inflation pressure and heart rate. The dose for 95% twitch suppression for gantacurium, CW002, cisatracurium, and rapacuronium was defined in the guinea pig. Transient and reproducible changes in pulmonary inflation pressure and heart rate were recorded after vagal nerve stimulation or intravenous injection of acetylcholine before and after pretreatment with cumulatively increasing concentrations of gantacurium, CW002, cisatracurium or a single concentration of rapacuronium.
The doses for 95% twitch suppression for gantacurium, CW002, cisatracurium, and rapacuronium were 0.064 +/- 0.006, 0.012 +/- 0.0006, 0.10 +/- 0.003, and 0.31 +/- 0.05 mg/kg, respectively. Gantacurium, CW002, and cisatracurium were without effects on baseline pulmonary inflation pressures and were devoid of significant interactions with M2 and M3 muscarinic receptors in vivo.
These findings suggest that gantacurium and CW002 are devoid of significant effects at airway muscarinic receptors particularly M3 receptors on bronchial smooth musculature at doses several fold higher than those required for functional muscle paralysis.
神经肌肉阻滞剂是全身麻醉的一个组成部分。除了它们在骨骼肌烟碱受体上的预期药理学靶标外,神经肌肉阻滞剂对气道毒蕈碱受体的亲和力还可能导致不理想的气道作用(即支气管收缩)。我们质疑 bisquaternary 非去极化肌松剂家族的两个新成员,即甘氨酰库铵和 CW002,在体内豚鼠气道模型中是否对气道毒蕈碱受体具有有害作用。
使用乌来坦麻醉的雄性豚鼠通过气管切开术进行通气,并连续记录肺充气压力和心率的数字记录。确定了甘氨酰库铵、CW002、顺式阿曲库铵和瑞库溴铵在豚鼠中的 95% 抽搐抑制剂量。在预先用累积增加浓度的甘氨酰库铵、CW002、顺式阿曲库铵或单次浓度的瑞库溴铵预处理后,在迷走神经刺激或静脉注射乙酰胆碱前后记录肺充气压力和心率的短暂和可重复变化。
甘氨酰库铵、CW002、顺式阿曲库铵和瑞库溴铵的 95% 抽搐抑制剂量分别为 0.064±0.006、0.012±0.0006、0.10±0.003 和 0.31±0.05mg/kg。甘氨酰库铵、CW002 和顺式阿曲库铵对基础肺充气压力没有影响,并且在体内对 M2 和 M3 毒蕈碱受体没有显著的相互作用。
这些发现表明,甘氨酰库铵和 CW002 在气道毒蕈碱受体上,特别是在支气管平滑肌上的 M3 受体上,在数倍于功能性肌肉麻痹所需的剂量下,没有明显的作用。