Fuster-Lluch Oscar, Zapater-Hernández Pedro, Gerónimo-Pardo Manuel
Clinical Chemistry Department, Hospital Universitari i Politècnic La Fe, Valencia, Spain.
Clinical Pharmacology Unit, Hospital General Universitario, Alicante, Spain.
J Clin Pharmacol. 2017 Oct;57(10):1345-1352. doi: 10.1002/jcph.903. Epub 2017 Apr 17.
The pharmacokinetic profile of intravenous acetaminophen administered to critically ill multiple-trauma patients was studied after 4 consecutive doses of 1 g every 6 hours. Eleven blood samples were taken (predose and 15, 30, 45, 60, 90, 120, 180, 240, 300, and 360 minutes postdose), and urine was collected (during 6-hour intervals between doses) to determine serum and urine acetaminophen concentrations. These were used to calculate the following pharmacokinetic parameters: maximum and minimum concentrations, terminal half-life, area under serum concentration-time curve from 0 to 6 hours, mean residence time, volume of distribution, and serum and renal clearance of acetaminophen. Daily doses of acetaminophen required to obtain steady-state minimum (bolus dosing) and average plasma concentrations (continuous infusion) of 10 μg/mL were calculated (10 μg/mL is the presumed lower limit of the analgesic range). Data are expressed as median [interquartile range]. Twenty-two patients were studied, mostly young (age 44 [34-64] years) males (68%), not obese (weight 78 [70-84] kg). Acetaminophen concentrations and pharmacokinetic parameters were these: maximum concentration 33.6 [25.7-38.7] μg/mL and minimum concentration 0.5 [0.2-2.3] μg/mL, all values below 10 μg/mL and 8 below the detection limit; half-life 1.2 [1.0-1.9] hours; area under the curve for 6 hours 34.7 [29.7-52.7] μg·h/mL; mean residence time 1.8 [1.3-2.6] hours; steady-state volume of distribution 50.8 [42.5-66.5] L; and serum and renal clearance 28.8 [18.9-33.7] L/h and 15 [11-19] mL/min, respectively. Theoretically, daily doses for a steady-state minimum concentration of 10 μg/mL would be 12.2 [7.8-16.4] g/day (166 [112-202] mg/[kg·day]); for an average steady-state concentration of 10 μg/mL, they would be 6.9 [4.5-8.1] g/day (91 [59-111] mg/[kg·day]). In conclusion, administration of acetaminophen at the recommended dosage of 1 g per 6 hours to critically ill multiple-trauma patients yields serum concentrations below 10 μg/mL due to increased elimination. To reach the 10 μg/mL target, and from a strictly pharmacokinetic point of view, continuous infusion may be more feasible than bolus dosing. Such a change in dosing strategy requires appropriate, pharmacokinetic-pharmacodynamic and specific safety study.
在对重症多发伤患者连续4次每6小时静脉注射1g对乙酰氨基酚后,研究了其药代动力学特征。采集了11份血样(给药前以及给药后15、30、45、60、90、120、180、240、300和360分钟),并收集尿液(在给药间隔的6小时内)以测定血清和尿液中对乙酰氨基酚的浓度。这些数据用于计算以下药代动力学参数:最大和最小浓度、终末半衰期、0至6小时血清浓度-时间曲线下面积、平均驻留时间、分布容积以及对乙酰氨基酚的血清清除率和肾清除率。计算了达到稳态最小(推注给药)和平均血浆浓度(持续输注)为10μg/mL所需的对乙酰氨基酚每日剂量(10μg/mL被认为是镇痛范围的下限)。数据以中位数[四分位间距]表示。研究了22例患者,大多数为年轻男性(年龄44[34 - 64]岁,占68%),非肥胖(体重78[70 - 84]kg)。对乙酰氨基酚浓度和药代动力学参数如下:最大浓度33.6[25.7 - 38.7]μg/mL,最小浓度0.5[0.2 - 2.3]μg/mL,所有值均低于10μg/mL,8个值低于检测限;半衰期1.2[1.0 - 1.9]小时;6小时曲线下面积34.7[29.7 - 52.7]μg·h/mL;平均驻留时间1.8[1.3 - 2.6]小时;稳态分布容积50.8[42.5 - 66.5]L;血清清除率和肾清除率分别为28.8[18.9 - 33.7]L/h和15[11 - 19]mL/min。理论上,达到稳态最小浓度10μg/mL的每日剂量为12.2[7.8 - 16.4]g/天(166[112 - 202]mg/[kg·天]);对于平均稳态浓度10μg/mL,每日剂量为6.9[4.5 - 8.1]g/天(91[59 - 111]mg/[kg·天])。总之,由于消除增加,以每6小时1g的推荐剂量对重症多发伤患者给予对乙酰氨基酚会使血清浓度低于10μg/mL。从严格的药代动力学角度来看,为达到10μg/mL的目标,持续输注可能比推注给药更可行。这种给药策略的改变需要进行适当的药代动力学-药效学和特定安全性研究。
Zotero 插件