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探索口服氯胺酮在接受烧伤手术儿童中的药代动力学。

Exploring the pharmacokinetics of oral ketamine in children undergoing burns procedures.

作者信息

Brunette Katharine E J, Anderson Brian J, Thomas Jennifer, Wiesner Lubbe, Herd David W, Schulein Simone

机构信息

Department of Anaesthesia, Auckland Children's Hospital, Auckland, New Zealand.

出版信息

Paediatr Anaesth. 2011 Jun;21(6):653-62. doi: 10.1111/j.1460-9592.2011.03548.x. Epub 2011 Feb 28.

Abstract

AIMS

The aim of this study was to describe ketamine pharmacokinetics when administered orally to children suffering from burn injury in >10% body surface area.

METHODS

Children (n = 20) were given ketamine 5 or 10 mg·kg(-1) orally 20 min prior to presentation for surgical procedures. Anesthesia during procedures was maintained with a volatile anesthetic agent. Additional intravenous ketamine was given as a bolus (0.5-1 mg·kg(-1)) to nine children during the procedure while a further nine children were given an infusion (0.1 mg·kg(-1)·h(-1)) continued for 4-19 h after the procedure. Blood was assayed for ketamine and norketamine on six occasions over the study duration of 8-24 h. Data were pooled with those from an earlier analysis (621 observations from 70 subjects). An additional time-concentration profile from an adult given oral ketamine was gleaned from the literature (17 observations). A population analysis was undertaken using nonlinear mixed-effects models.

RESULTS

The pooled analysis comprised 852 observations from 91 subjects. There were 20 children who presented for procedures related to burns management (age 3.5 sd 2.1 years, range 1-8 years; weight 14.7 sd 4.9 kg, range 7.9-25 kg), and these children contributed 214 ketamine and norketamine observations. A two-compartment (central, peripheral) linear disposition model fitted data better than a one-compartment model. Bioavailability of the oral formulation was 0.45 (90% CI 0.33, 0.58). Absorption half-time was 59 (90% CI 29.4, 109.2) min and had high between-subject variability (BSV 148%). Population parameter estimates, standardized to a 70-kg person, were central volume 21.1 (BSV 47.1%) l·70 kg(-1), peripheral volume of distribution 109 (27.5%) l·70 kg(-1), clearance 81.3 (46.1%) l·h(-1)·70 kg(-1), and inter-compartment clearance 259 (50.1%) l·h(-1)·70 kg(-1). Under the assumption that all ketamine was converted to norketamine, the volume of the metabolite was 151.9 (BSV 39.1%) l·70 kg(-1) with an elimination clearance of 64.4 (BSV 63.4%) l·h(-1) ·70 kg(-1) and a rate constant for intermediate compartments of 26.2 (BSV 52.1%) h(-1)·70 kg(-1).

CONCLUSIONS

The ketamine pharmacokinetics in children with minor burns are similar to those without burns. The peak ratio of norketamine/ketamine at 1 h is 2.8 after oral administration allowing an analgesic contribution from the metabolite at this time. There is low relative bioavailability (<0.5) and slow variable absorption. Dose simulation in a child (3.5 years, 15 kg) suggests a dose regimen of oral ketamine 10 mg·kg(-1) followed by intravenous ketamine 1 mg·kg(-1) i.v. with the advent of short-duration surgical dressing change at 45 min.

摘要

目的

本研究旨在描述口服氯胺酮在烧伤面积超过体表面积10%的儿童中的药代动力学。

方法

20名儿童在接受外科手术前20分钟口服5或10mg·kg⁻¹氯胺酮。手术期间使用挥发性麻醉剂维持麻醉。9名儿童在手术过程中静脉推注额外的氯胺酮(0.5 - 1mg·kg⁻¹),另外9名儿童在手术后接受持续4 - 19小时的输注(0.1mg·kg⁻¹·h⁻¹)。在8 - 24小时的研究期间,六次采集血液检测氯胺酮和去甲氯胺酮。数据与早期分析的数据(来自70名受试者的621次观察)合并。从文献中收集了一名成年人口服氯胺酮的额外时间 - 浓度曲线(17次观察)。使用非线性混合效应模型进行群体分析。

结果

汇总分析包括来自91名受试者的852次观察。有20名儿童因烧伤处理相关手术前来就诊(年龄3.5±2.1岁,范围1 - 8岁;体重14.7±4.9kg,范围7.9 - 25kg),这些儿童提供了214次氯胺酮和去甲氯胺酮观察数据。二室(中央室、外周室)线性处置模型比一室模型更能拟合数据。口服制剂的生物利用度为0.45(90%CI 0.33,0.58)。吸收半衰期为59(90%CI 29.4,109.2)分钟,个体间变异性高(个体间变异系数148%)。以70kg个体标准化的群体参数估计值为:中央室容积21.1(个体间变异系数47.1%)l·70kg⁻¹,外周分布容积109(27.5%)l·70kg⁻¹,清除率81.3(46.1%)l·h⁻¹·70kg⁻¹,室间清除率259(50.1%)l·h⁻¹·70kg⁻¹。假设所有氯胺酮都转化为去甲氯胺酮,代谢产物的容积为151.9(个体间变异系数39.1%)l·70kg⁻¹,消除清除率为64.4(个体间变异系数63.4%)l·h⁻¹·70kg⁻¹,中间室的速率常数为26.2(个体间变异系数52.1%)h⁻¹·70kg⁻¹。

结论

轻度烧伤儿童的氯胺酮药代动力学与未烧伤儿童相似。口服给药后1小时去甲氯胺酮/氯胺酮的峰值比为2.8,此时代谢产物有镇痛作用。相对生物利用度低(<0.5)且吸收缓慢且可变。对一名3.5岁、15kg儿童的剂量模拟表明,在45分钟进行短期手术换药时,口服氯胺酮10mg·kg⁻¹后静脉注射氯胺酮1mg·kg⁻¹的给药方案。

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