Wiest D
Medical University of South Carolina, College of Pharmacy, Charleston, USA.
Clin Pharmacokinet. 1995 Mar;28(3):190-202. doi: 10.2165/00003088-199528030-00002.
Esmolol is an ultra short-acting intravenous cardioselective beta-antagonist. It has an extremely short elimination half-life (mean: 9 minutes; range: 4 to 16 minutes) and a total body clearance [285 ml/min/kg (17.1 L/h/kg)] approaching 3 times cardiac output and 14 times hepatic blood flow. The alpha-distribution half-life is approximately 2 minutes. When esmolol is administered as a bolus followed by a continuous infusion, onset of activity occurs within 2 minutes, with 90% of steady-state beta-blockade occurring within 5 minutes. Full recovery from beta-blockade is observed 18 to 30 minutes after terminating the infusion. Esmolol blood concentrations are undetectable 20 to 30 minutes postinfusion. The elimination of esmolol is independent of renal or hepatic function as it is metabolised by red blood cell cytosol esterases to an acid metabolite and methanol. The acid metabolite, which is renally eliminated, has 1500-fold less activity than esmolol. Methanol concentrations remain within the range of normal endogenous levels. Clinically, esmolol is used for the following: (i) situations where a brief duration of adrenergic blockade is required, such as tracheal intubation and stressful surgical stimuli; and (ii) critically ill or unstable patients in whom the dosage of esmolol is easily titrated to response and adverse effects are rapidly managed by termination of the infusion. In adults, bolus doses of 100 to 200mg are effective in attenuating the adrenergic responses associated with tracheal intubation and surgical stimuli. For the control of supraventricular arrhythmias, acute postoperative hypertension and acute ischaemic heart disease, doses of < 300 micrograms/kg/min, administered by continuous intravenous infusion, are used. The principal adverse effect of esmolol is hypotension (incidence of 0 to 50%), which is frequently accompanied with diaphoresis. The incidence of hypotension appears to increase with doses exceeding 150 micrograms/kg/min and in patients with low baseline blood pressure. Hypotension infrequently requires any intervention other than decreasing the dose or discontinuing the infusion. Symptoms generally resolve within 30 minutes after discontinuing the drug. In surgical and critical care settings where clinical conditions are rapidly changing, the pharmacokinetic profile of esmolol allows the drug to provide rapid pharmacological control and minimises the potential for serious adverse effects.
艾司洛尔是一种超短效静脉注射用心脏选择性β受体拮抗剂。其消除半衰期极短(平均:9分钟;范围:4至16分钟),全身清除率为[285毫升/分钟/千克(17.1升/小时/千克)],接近心输出量的3倍和肝血流量的14倍。α分布半衰期约为2分钟。当静脉推注艾司洛尔后接着持续输注时,2分钟内起效,5分钟内达到稳态β受体阻滞的90%。输注结束后18至30分钟可观察到β受体阻滞的完全恢复。输注后20至30分钟检测不到艾司洛尔的血药浓度。艾司洛尔的消除不依赖于肾或肝功能,因为它由红细胞胞质酯酶代谢为一种酸性代谢产物和甲醇。该酸性代谢产物经肾脏排泄,其活性比艾司洛尔低1500倍。甲醇浓度保持在正常内源性水平范围内。临床上,艾司洛尔用于以下情况:(i)需要短暂肾上腺素能阻滞的情况,如气管插管和应激性手术刺激;(ii)病情危重或不稳定的患者,此类患者中艾司洛尔的剂量易于根据反应进行滴定,且通过停止输注可迅速控制不良反应。在成人中,100至200毫克的静脉推注剂量可有效减轻与气管插管和手术刺激相关的肾上腺素能反应。为控制室上性心律失常、术后急性高血压和急性缺血性心脏病,采用持续静脉输注,剂量<300微克/千克/分钟。艾司洛尔的主要不良反应是低血压(发生率为0至50%),常伴有多汗。当剂量超过150微克/千克/分钟以及基线血压较低的患者中,低血压的发生率似乎会增加。低血压很少需要除降低剂量或停止输注以外的任何干预措施。停药后症状通常在30分钟内缓解。在临床情况迅速变化的手术和重症监护环境中,艾司洛尔的药代动力学特征使该药物能够提供快速的药理控制,并将严重不良反应的可能性降至最低。
