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艾司洛尔对麻醉状态下人体的心血管效应。

Cardiovascular effects of esmolol in anesthetized humans.

作者信息

Menkhaus P G, Reves J G, Kissin I, Alvis J M, Govier A V, Samuelson P N, Lell W A, Henling C E, Bradley E

出版信息

Anesth Analg. 1985 Mar;64(3):327-34.

PMID:2858169
Abstract

We studied the cardiovascular effects of esmolol, a newly synthesized beta-adrenocepter antagonist, in anesthetized humans. Forty patients (four groups of 10 each) with ischemic heart disease and normal ventricular function were anesthetized with diazepam, pancuronium, and N2O in O2. Esmolol was given by continuous infusion in cumulative doses of 1100 micrograms/kg (group 1), 2000 micrograms/kg (group 2), and 2700 micrograms/kg (group 3); a control group received no esmolol. Infusion of esmolol was begun 3 min prior to and ended 4 min after tracheal intubation. All three doses of esmolol significantly (P less than 0.001) attenuated the heart rate responses to intubation. Rate-pressure products were significantly (P less than 0.001) lower in esmolol-treated patients than in controls after intubation, but ST-segment changes compatible with ischemia occurred in one patient in each group. Increases in heart rate were associated with significant increases in plasma norepinephrine levels (r = 0.45, P = 0.02) in the control group, but not in esmolol-treated patients, a demonstration that esmolol antagonizes the beta-adrenergic effects of norepinephrine. The effect of esmolol on heart rate was absent 5 min after cessation of infusion, and plasma levels of esmolol were undetectable in 26 of 30 treated patients 15 min after the termination of esmolol infusion. Esmolol has a rapid onset and short duration of effect. It can be used safely during anesthesia in patients with normal ventricular function to attenuate cardiac response to sympathetic stimulation.

摘要

我们在麻醉的人体中研究了新合成的β-肾上腺素能受体拮抗剂艾司洛尔对心血管系统的影响。40例患有缺血性心脏病且心室功能正常的患者(分为4组,每组10例),用安定、泮库溴铵和氧气与笑气混合气体进行麻醉。艾司洛尔以累积剂量1100微克/千克(第1组)、2000微克/千克(第2组)和2700微克/千克(第3组)持续输注;对照组未给予艾司洛尔。在气管插管前3分钟开始输注艾司洛尔,并在气管插管后4分钟结束。所有三个剂量的艾司洛尔均显著(P<0.001)减弱了插管引起的心率反应。插管后,接受艾司洛尔治疗的患者的心率-血压乘积显著(P<0.001)低于对照组,但每组均有1例患者出现与缺血相符的ST段改变。对照组中,心率增加与血浆去甲肾上腺素水平显著升高相关(r = 0.45,P = 0.02),但在接受艾司洛尔治疗的患者中并非如此,这表明艾司洛尔可拮抗去甲肾上腺素的β-肾上腺素能效应。输注停止5分钟后,艾司洛尔对心率的作用消失,在艾司洛尔输注结束15分钟后,30例接受治疗的患者中有26例检测不到血浆艾司洛尔水平。艾司洛尔起效迅速,作用持续时间短。它可安全用于心室功能正常的患者麻醉期间,以减弱心脏对交感神经刺激的反应。

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