新斯的明和依酚氯铵在猫体内引起的心动过缓的不同特性。

Different properties of the bradycardia produced by neostigmine and edrophonium in the cat.

作者信息

Backman S B, Stein R D, Blank D W, Collier B, Polosa C

机构信息

Department of Anaesthesia, Royal Victoria Hospital, Montreal, Quebec, Canada.

出版信息

Can J Anaesth. 1996 Jul;43(7):731-40. doi: 10.1007/BF03017959.

DOI:10.1007/BF03017959

PMID:8807181

Abstract

PURPOSE

The bradycardia produced by neostigmine and edrophonium was examined according to its relation to cholinesterase inhibition and to its sensitivity to block by muscarinic receptor antagonists. For comparison, the ability of muscarinic antagonists to block the bradycardia produced by electrical stimulation of the vagus nerve was determined.

METHODS

Cats were anaesthetized, vagotomized and propranolol-treated. Heart rate was continuously recorded. Erythrocyte cholinesterase activity of arterial blood was measured using a radiometric technique. The right vagus nerve was isolated for electrical stimulation. The muscarinic antagonists used were atropine, glycopyrrolate, pancuronium, gallamine, and AFDX-116.

RESULTS

Neostigmine produced a dose-dependent decrease in cholinesterase activity which reached a plateau at a cumulative dose of 0.16 mg.kg-1 (ED50 0.009 +/- 0.003 mg.kg-1). Neostigmine produced a dose-dependent decrease in heart rate with the dose-response relationship (ED50 0.1 +/- 0.01 mg.kg-1; P = 0.0006) shifted to the right of that for the inhibition of cholinesterase activity. In contrast to the anticholinesterase effect, the bradycardic effect did not reach a plateau and continued to increase even at doses at which the cholinesterase inhibition was maximal. The maximal decrease in heart rate when the heart was still in sinus rhythm was by 81 +/- 13 bpm (49 +/- 7% of baseline), which was produced by a dose of 0.32 mg.kg-1. Edrophonium produced dose-dependent decreases in cholinesterase activity and heart rate, which were highly correlated (correlation coefficient r = 0.99, P < 0.0001). The ED50 of the reduction in heart rate (0.9 +/- 0.18 mg.kg-1) and cholinesterase activity (0.89 +/- 0.12 mg.kg-1) produced by edrophonium were similar. Moreover, the reduction in heart rate and cholinesterase activity produced by edrophonium reached a plateau at the same dose (6.4 mg.kg-1). At this dose, heart rate decreased by 22 +/- 2 bpm (14.6 +/- 0.9% of baseline). Compared to the bradycardia produced by stimulation of the vagus nerve, that produced by neostigmine was blocked by muscarinic antagonists at significantly lower doses while that produced by edrophonium was blocked at similar doses.

CONCLUSIONS

The neostigmine-induced bradycardia is poorly correlated with cholinesterase inhibition compared to that produced by edrophonium, and has a higher sensitivity to muscarinic receptor antagonists compared to that produced by edrophonium or vagus nerve stimulation. These results are consistent with the hypothesis that the neostigmine-induced bradycardia is, in part, the result of neostigmine directly activating cholinergic receptors within the cardiac parasympathetic pathway. The bradycardia produced by edrophonium may be accounted for solely by an anticholinesterase action.

摘要

目的

根据新斯的明和依酚氯铵所致心动过缓与胆碱酯酶抑制的关系及其对毒蕈碱受体拮抗剂阻断作用的敏感性，对其进行研究。为作比较，测定了毒蕈碱拮抗剂阻断迷走神经电刺激所致心动过缓的能力。

方法

将猫麻醉、切断迷走神经并给予普萘洛尔治疗。连续记录心率。采用放射性技术测定动脉血红细胞胆碱酯酶活性。分离右侧迷走神经用于电刺激。所用的毒蕈碱拮抗剂有阿托品、格隆溴铵、泮库溴铵、加拉明和AFDX - 116。

结果

新斯的明使胆碱酯酶活性呈剂量依赖性降低，累积剂量达0.16mg·kg⁻¹时达到平台期（半数有效量[ED50]为0.009±0.003mg·kg⁻¹）。新斯的明使心率呈剂量依赖性降低，其剂量 - 反应关系（ED50为0.1±0.01mg·kg⁻¹；P = 0.0006）向右移至胆碱酯酶活性抑制的剂量 - 反应关系的右侧。与抗胆碱酯酶作用相反，心动过缓作用未达到平台期，即使在胆碱酯酶抑制作用最大的剂量下仍继续增加。心脏仍处于窦性心律时，心率最大降低值为81±13次/分（为基线值的49±7%），此为剂量0.32mg·kg⁻¹所致。依酚氯铵使胆碱酯酶活性和心率呈剂量依赖性降低，二者高度相关（相关系数r = 0.99，P < 0.0001）。依酚氯铵所致心率降低（0.9±0.18mg·kg⁻¹）和胆碱酯酶活性降低（0.89±0.12mg·kg⁻¹）的ED50相似。此外，依酚氯铵所致心率降低和胆碱酯酶活性降低在相同剂量（6.4mg·kg⁻¹）时达到平台期。在此剂量下，心率降低22±2次/分（为基线值的14.6±0.9%）。与迷走神经刺激所致心动过缓相比，新斯的明所致心动过缓被毒蕈碱拮抗剂阻断时所需剂量显著更低，而依酚氯铵所致心动过缓被阻断时所需剂量相似。

结论

与依酚氯铵所致心动过缓相比，新斯的明所致心动过缓与胆碱酯酶抑制的相关性较差，且与依酚氯铵或迷走神经刺激所致心动过缓相比，对毒蕈碱受体拮抗剂更为敏感。这些结果与以下假说一致，即新斯的明所致心动过缓部分是新斯的明直接激活心脏副交感神经通路内胆碱能受体的结果。依酚氯铵所致心动过缓可能仅由抗胆碱酯酶作用引起。