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一种用于麻醉和镇静的瑞马唑仑药代动力学和药效学模型的开发与分析,并提出给药方案和浓度建议。

Development and analysis of a remimazolam pharmacokinetics and pharmacodynamics model with proposed dosing and concentrations for anaesthesia and sedation.

作者信息

Eleveld Douglas J, Colin Pieter J, Van den Berg Johannes P, Koomen Jeroen V, Stoehr Thomas, Struys Michel M R F

机构信息

Department of Anesthesiology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands.

Department of Anesthesiology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands.

出版信息

Br J Anaesth. 2025 Jul;135(1):206-217. doi: 10.1016/j.bja.2025.02.038. Epub 2025 Apr 30.

DOI:10.1016/j.bja.2025.02.038
PMID:40312166
Abstract

BACKGROUND

Pharmacokinetic-pharmacodynamic (PK-PD) models of remimazolam and their covariate relationships are useful for understanding drug disposition and predicting drug effects. Although clinical studies have shown that remimazolam induction doses decline with advancing age, this property is not reflected in existing models. The purpose of this investigation was to develop a PK-PD model for remimazolam and perform covariate analysis to maximise its utility across broad, diverse populations and to evaluate its consistency with clinical observations of drug dosing.

METHODS

Arterial and venous concentrations of remimazolam and its metabolite, Modified Observer's Assessment of Alertness and Sedation score and bispectral index were determined in 20 studies. Final population models were developed with covariate analysis. Simulations of drug administration for sedation and anaesthesia for this and previously published models were compared with the results of clinical studies.

RESULTS

Model development proceeded from 933 individuals aged 6-93 yr and weight 21-171 kg. PK data from studies with extracorporeal membrane oxygenation and treatment in ICU were considered in a post hoc analysis. Simulations of target-controlled infusion with the final model targeting sedation (Modified Observer's Assessment of Alertness and Sedation score 2 or 3) or anaesthesia (bispectral index 50) showed drug administration declining with age consistent with clinical observations.

CONCLUSIONS

A PK-PD model for remimazolam was developed for a broad, diverse population. Dosing and target concentrations are proposed that are clinically useful for anaesthesia and sedation, especially for target-controlled infusion administration.

摘要

背景

瑞马唑仑的药代动力学-药效学(PK-PD)模型及其协变量关系有助于理解药物处置过程并预测药物效应。尽管临床研究表明瑞马唑仑诱导剂量会随着年龄增长而下降,但现有模型并未体现这一特性。本研究的目的是建立瑞马唑仑的PK-PD模型,并进行协变量分析,以在广泛多样的人群中最大化其效用,并评估其与药物给药临床观察结果的一致性。

方法

在20项研究中测定了瑞马唑仑及其代谢产物的动脉血和静脉血浓度、改良警觉/镇静评分以及脑电双频指数。通过协变量分析建立最终的群体模型。将该模型以及之前发表的模型用于镇静和麻醉给药的模拟结果与临床研究结果进行比较。

结果

模型构建纳入了933名年龄在6至93岁、体重在21至171千克的个体。在一项事后分析中考虑了来自体外膜肺氧合和重症监护病房治疗研究的PK数据。使用最终模型进行目标浓度输注模拟,目标为镇静(改良警觉/镇静评分为2或3)或麻醉(脑电双频指数为50),结果显示给药量随年龄下降,与临床观察结果一致。

结论

为广泛多样的人群建立了瑞马唑仑的PK-PD模型。提出了在麻醉和镇静中具有临床实用性的给药剂量和目标浓度,特别是对于目标浓度输注给药。

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