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择期开颅手术患者中推注甘露醇的药代动力学特征。

Pharmacokinetic characteristics of bolus-administered mannitol in patients undergoing elective craniotomy.

机构信息

Department of Anesthesia, University of Iowa Roy J. and Lucille A. Carver College of Medicine, 200 Hawkins Drive 6504-1 JCP, Iowa City, IA 52242, USA.

出版信息

J Clin Pharmacol. 2010 May;50(5):536-43. doi: 10.1177/0091270009348973. Epub 2010 Jan 5.

Abstract

To better understand mannitol pharmacokinetics, the authors constructed and compared population models for high-versus low-dose bolus infusions in humans. Patients (aged 18-75, American Society of Anesthesiologists physical status 1-3) scheduled for elective craniotomy with an anticipated need for intraoperative mannitol were randomly assigned to receive either 0.5 (n = 10) or 1.0 (n = 12) g/kg of 20% mannitol over 15 minutes. Serial blood samples were collected at the predetermined intervals over 12 hours. Plasma mannitol concentrations were measured by gas chromatography and subjected to pharmacokinetic analysis; a 3-compartment model best described mannitol disposition characteristics. Weight and dose were the important covariates for rapid peripheral volume of distribution (V2) and central clearance (CL1), respectively. Estimated population means were 2.80, 8.86, and 12.0 L for central (V1), rapid (V2), and slow (V3) volumes of distribution, respectively. Clearances of the central compartments (CL1) were 0.07 versus 0.04 L/min in the high-versus low-dose group, respectively. Thus, mannitol kinetics can be considered as nonlinear. Clearances of the rapid peripheral (CL2) and slow peripheral compartments (CL3) were identical (2.07 and 0.16 L/min) in both. The current weight-based dosing guidelines yielded greater than expected plasma drug concentrations in obese patients.

摘要

为了更好地了解甘露醇药代动力学,作者构建并比较了高剂量与低剂量快速推注在人体中的群体模型。择期行开颅术且术中预计需要甘露醇的患者(年龄 18-75 岁,美国麻醉医师协会身体状况 1-3 级),按 0.5 g/kg(n = 10)或 1.0 g/kg(n = 12)20%甘露醇 15 分钟快速推注的方案进行随机分组。在 12 小时内的预定时间间隔采集连续血样。采用气相色谱法测定血浆甘露醇浓度,并进行药代动力学分析;3 室模型最能描述甘露醇的分布特征。体重和剂量分别是快速外周分布容积(V2)和中央清除率(CL1)的重要协变量。群体平均值分别为中央(V1)、快速(V2)和缓慢(V3)分布容积的 2.80、8.86 和 12.0 L。中央室(CL1)的清除率在高剂量与低剂量组分别为 0.07 和 0.04 L/min。因此,甘露醇动力学可以被认为是非线性的。快速外周(CL2)和缓慢外周(CL3)的清除率在两组中相同(分别为 2.07 和 0.16 L/min)。目前基于体重的给药指南导致肥胖患者的血浆药物浓度高于预期。

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