瑞芬太尼在重症肝病志愿者受试者中的药代动力学和药效学。

Pharmacokinetics and pharmacodynamics of remifentanil in volunteer subjects with severe liver disease.

作者信息

Dershwitz M, Hoke J F, Rosow C E, Michałowski P, Connors P M, Muir K T, Dienstag J L

机构信息

Department of Anesthesia, Massachusetts General Hospital and Harvard Medical School, Boston, USA.

出版信息

Anesthesiology. 1996 Apr;84(4):812-20. doi: 10.1097/00000542-199604000-00008.

DOI:10.1097/00000542-199604000-00008

PMID:8638835

Abstract

BACKGROUND

Remifentanil, a new mu-opioid agonist with an extremely short duration of action, is metabolized by circulating and tissue esterases; therefore, its clearance should be relatively unaffected by changes in hepatic or renal function. This study was designed to determine whether severe hepatic disease affects the pharmacokinetics or pharmacodynamics of remifentanil.

METHODS

Ten volunteers with chronic, stable, severe hepatic disease and awaiting liver transplantation and ten matched controls were enrolled. Each subject was given a 4-h infusion of remifentanil. The first five pairs received 0.0125 microgram x kg(-1) x min(-1) for 1 h followed by 0.025 microgram x kg(-1) x min(-1) for 3 h; the second five pairs received double these infusion rates. During and after the infusion, arterial blood was obtained for pharmacokinetic analyses, and the ventilatory response to a hypercarbic challenge was assessed. Simultaneous pharmacokinetic and pharmacodynamic analyses were performed. The pharmacokinetics were described using a one-compartment intravenous infusion model, and ventilatory depression was modelled using the inhibitory E(max) model. The pharmacokinetics of the metabolite GR90291 were determined using noncompartmental methods.

RESULTS

There were no differences in any of the pharmacokinetic parameters for remifentanil or GR90291 between the two groups. The subjects with liver disease were more sensitive to the ventilatory depressant effects of remifentanil. The EC(50) values (the remifentanil concentrations determined from simultaneous pharmacokinetic/pharmacodynamic analyses to depress carbon dioxide-stimulated minute ventilation by 50%) in the control and hepatic disease groups were 2.52 ng/ml (95% confidence interval 2.07-2.97 ng/ml) and 1.56 ng/ml (95% confidence interval 1.37-1.76 ng/ml), respectively.

CONCLUSIONS

The pharmacokinetics of remifentanil and GR90291 are unchanged in persons with severe, chronic liver disease. Such patients may be more sensitive to the ventilatory depressant effects of remifentanil, a finding of uncertain clinical significance, considering the extremely short duration of action of the drug.

摘要

背景

瑞芬太尼是一种新型μ阿片受体激动剂，作用持续时间极短，经循环和组织酯酶代谢；因此，其清除率相对不受肝肾功能变化的影响。本研究旨在确定严重肝病是否会影响瑞芬太尼的药代动力学或药效动力学。

方法

招募了10名患有慢性、稳定、严重肝病且等待肝移植的志愿者以及10名匹配的对照组。每位受试者接受4小时的瑞芬太尼输注。前五对受试者以0.0125微克·千克⁻¹·分钟⁻¹的速率输注1小时，随后以0.025微克·千克⁻¹·分钟⁻¹的速率输注3小时；后五对受试者接受的输注速率为上述速率的两倍。在输注期间和之后，采集动脉血进行药代动力学分析，并评估对高碳酸血症刺激的通气反应。进行了同时的药代动力学和药效动力学分析。药代动力学采用一室静脉输注模型描述，通气抑制采用抑制性E(max)模型建模。代谢物GR90291的药代动力学采用非房室方法测定。

结果

两组之间瑞芬太尼或GR90291的任何药代动力学参数均无差异。肝病患者对瑞芬太尼的通气抑制作用更敏感。对照组和肝病组的EC(50)值（通过同时的药代动力学/药效动力学分析确定的使二氧化碳刺激的分钟通气量降低50%的瑞芬太尼浓度）分别为2.52纳克/毫升（95%置信区间2.07 - 2.97纳克/毫升）和1.56纳克/毫升（95%置信区间1.37 - 1.76纳克/毫升）。