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成人静脉利多卡因的群体药代动力学:系统评价。

Population Pharmacokinetics of Intravenous Lidocaine in Adults: A Systematic Review.

机构信息

Department of Anaesthesiology, Faculty of Medicine, Universiti Malaya, 50603, Kuala Lumpur, Malaysia.

Department of Pharmacy Practice, School of Pharmacy, International Medical University, No. 126, Jalan Jalil Perkasa 19, Bukit Jalil, 57000, Kuala Lumpur, Malaysia.

出版信息

Clin Pharmacokinet. 2024 May;63(5):623-643. doi: 10.1007/s40262-024-01373-4. Epub 2024 May 4.

Abstract

BACKGROUND

The establishment of optimal dosing regimens for intravenous (IV) lidocaine in the perioperative setting, aiming to balance effective pain relief with minimisation of potential side effects, is a topic of ongoing debate. This discussion stems from the significant variability in lidocaine's pharmacokinetic (PK) parameters and its relatively narrow safety margin. Population pharmacokinetic (popPK) modelling has emerged as a valuable tool for understanding the factors contributing to this observed variability in drug kinetics.

OBJECTIVES

This systematic review compiles the existing knowledge on lidocaine's PK properties and published popPK models, with a focus on significant covariates.

METHODS

A systematic search on Cochrane CENTRAL, Medline, and EMBASE was performed from inception to June 2023. Original clinical studies that administered IV lidocaine to adults and performed PK analyses using a nonlinear mixed effects modelling approach were included. The quality of the included studies was assessed by compliance with the Clinical Pharmacokinetics (ClinPK) statement checklist.

RESULTS

Seven studies were included, which involved a diverse adult population, including both volunteers and patients with various comorbidities. Lidocaine PK was primarily characterised by a two- or three-compartment model. The volume of distribution at steady state ranged from 66 to 194 L, and the total clearance ranged from 22 to 49 L/h. Despite adjusting for significant covariates like heart failure status, alpha-1-acid glycoprotein, duration of lidocaine infusion, and body weight, each study revealed substantial variability in PK parameters. The potential impact of hepatic or renal function biomarkers on these PK parameters calls for further investigation. Incomplete reporting of key aspects of developed models may hinder the models' reliability and clinical application.

CONCLUSION

The findings emphasise the importance of tailoring drug dosage to ensure the safe and effective use of intravenous lidocaine. Optimal design methodologies may be incorporated for a more efficient identification of important covariates. Utilising contemporary model evaluation methods like visual predictive checks and bootstrapping would enhance the robustness of popPK models and the reliability of their predictions. This comprehensive review advances our understanding of lidocaine's pharmacokinetics and lays the groundwork for further research in this critical area of perioperative pain management. Review protocol registered on 25 August 2023 in PROSPERO (CRD42023441113). This work was supported by the Fundamental Research Grant Scheme, the Ministry of Higher Education, Malaysia (FRGS/1/2020/SKK01/UM/02/2).

摘要

背景

在围手术期建立静脉(IV)利多卡因的最佳剂量方案,旨在平衡有效止痛与最小化潜在副作用,这是一个持续争论的话题。这一讨论源于利多卡因药代动力学(PK)参数的显著变异性及其相对较窄的安全范围。群体药代动力学(popPK)建模已成为理解药物动力学观察到的变异性的重要工具。

目的

本系统综述总结了利多卡因 PK 特性和已发表的 popPK 模型的现有知识,重点关注重要协变量。

方法

从创建到 2023 年 6 月,在 Cochrane 中央、Medline 和 EMBASE 上进行了系统搜索。纳入了向成人静脉内给予利多卡因并使用非线性混合效应建模方法进行 PK 分析的原始临床研究。通过遵守临床药代动力学(ClinPK)声明检查表评估纳入研究的质量。

结果

纳入了 7 项研究,涉及到包括志愿者和伴有各种合并症的患者在内的多样化成年人群体。利多卡因 PK 主要以二或三房室模型为特征。稳态时的分布容积范围为 66 至 194 L,总清除率范围为 22 至 49 L/h。尽管对心力衰竭状态、α-1-酸性糖蛋白、利多卡因输注时间和体重等重要协变量进行了调整,但每个研究都显示出 PK 参数的显著变异性。肝或肾功能生物标志物对这些 PK 参数的潜在影响需要进一步研究。开发模型的关键方面报告不完整可能会影响模型的可靠性和临床应用。

结论

研究结果强调了为确保静脉内利多卡因的安全有效使用而调整药物剂量的重要性。可以采用最佳设计方法来更有效地确定重要协变量。利用现代模型评估方法,如可视化预测检查和自举,将提高 popPK 模型的稳健性和预测的可靠性。本综述全面了解了利多卡因的药代动力学,并为围手术期疼痛管理这一关键领域的进一步研究奠定了基础。综述方案于 2023 年 8 月 25 日在 PROSPERO(CRD42023441113)上注册。这项工作得到了马来西亚高等教育部基础研究基金计划(FRGS/1/2020/SKK01/UM/02/2)的支持。

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