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健康志愿者在全身麻醉前和麻醉期间去甲肾上腺素的群体药代动力学模型建立。

Population Pharmacokinetic Modelling of Norepinephrine in Healthy Volunteers Prior to and During General Anesthesia.

机构信息

Department of Anaesthesiology, University Medical Center Groningen, University of Groningen, Hanzeplein 1, 9713 GZ, Groningen, The Netherlands.

Department of Pharmacology, Toxicology and Kinetics, CBG-MEB, Utrecht, The Netherlands.

出版信息

Clin Pharmacokinet. 2024 Nov;63(11):1597-1608. doi: 10.1007/s40262-024-01430-y. Epub 2024 Oct 27.

Abstract

BACKGROUND

Intraoperation hypotension (IOH) is commonly observed in patients undergoing surgery under general anesthesia, and even a brief episode of IOH can lead to unfavorable outcomes. To reduce the risk, blood pressure is closely measured during general anesthesia, and norepinephrine (NE) is frequently administered if hypotension is detected. Despite its routine application, information on the dose-exposure-response relationship of NE remains limited. Additionally, quantification of the influence of general anesthesia on the pharmacokinetics (PK) of NE is lacking.

OBJECTIVE

In this study, we aimed to describe NE PK in healthy volunteers and the influence of general anesthesia on its PK.

METHODS

A single-center, cross-over study was conducted in healthy volunteers. The volunteers received a step-up NE dosing scheme (0.04, 0.08, 0.12, 0.16 and 0.20 mcg/kg/min) first in the awake state and then under general anesthesia. General anesthesia was administered using a propofol/remifentanil Eleveld target-controlled infusion. During general anesthesia, a 30-second electrical stimulus was given as surrogate for surgical incision to the volunteers at each dosage step. Blood samples were drawn before the initial dosing and after each dosing step, and plasma NE, propofol and remifentanil concentrations were subsequently determined. A population PK model was developed using non-linear mixed effects modelling. Simulations were conducted to predict the plasma NE concentration in patients at different measured propofol concentrations.

RESULTS

A total of 1219 samples were analyzed from 36 volunteers. A two-compartment model with a first-order elimination best described the data. Weight, age, and session effect (awake vs general anesthesia) were identified as relevant covariates on the clearance (CL) of NE. A 10% decrease in NE CL was observed after general anesthesia induction. This difference between sessions is better explained by the measured concentration of propofol, rather than the anticipated impact of cardiac output. The estimated post-stimulation NE concentration is 0.66 nmol/L (95% CI 0.06-1.20 nmol/L) lower than the pre-stimulation NE concentration. Model simulation indicates that patients at a higher measured propofol concentration (e.g., 6 mcg/mL) exhibited higher NE concentrations (95% PI 18.10-43.89 nmol/L) than patients at a lower measured propofol concentration (e.g., 3 mcg/mL) (95% PI 16.81-38.91 nmol L).

CONCLUSION

The NE PK is well described with a two-compartment model with a first-order elimination. NE CL exhibiting a 10% decrease under general anesthesia, with this difference being attributed to the measured concentration of propofol. The impact of stimulation on NE PK under general anesthesia is very limited.

CLINICAL TRIALS REGISTRATION NUMBER

NL9312.

摘要

背景

术中低血压(IOH)在全身麻醉下接受手术的患者中很常见,即使是短暂的 IOH 发作也可能导致不良后果。为了降低风险,在全身麻醉期间密切测量血压,如果发现低血压则经常给予去甲肾上腺素(NE)。尽管它是常规应用的,但有关 NE 的剂量-暴露-反应关系的信息仍然有限。此外,缺乏对全身麻醉对 NE 药代动力学(PK)影响的量化。

目的

本研究旨在描述健康志愿者中的 NE PK 以及全身麻醉对其 PK 的影响。

方法

一项在健康志愿者中进行的单中心、交叉研究。志愿者首先在清醒状态下接受逐步递增的 NE 剂量方案(0.04、0.08、0.12、0.16 和 0.20 mcg/kg/min),然后在全身麻醉下接受 NE 剂量方案。全身麻醉采用丙泊酚/瑞芬太尼 Eleveld 靶控输注。在全身麻醉期间,志愿者在每个剂量步骤中接受 30 秒的电刺激作为手术切口的替代物。在初始给药前和每次给药后抽取血样,并随后测定血浆 NE、丙泊酚和瑞芬太尼浓度。使用非线性混合效应建模开发了群体 PK 模型。进行模拟以预测不同测量丙泊酚浓度下患者的血浆 NE 浓度。

结果

共对 36 名志愿者的 1219 个样本进行了分析。具有一阶消除的两室模型最能描述数据。体重、年龄和会话效应(清醒与全身麻醉)被确定为 NE 清除率(CL)的相关协变量。全身麻醉诱导后,NE CL 降低了 10%。这种会话之间的差异更好地解释为测量的丙泊酚浓度,而不是预期的心脏输出的影响。刺激后的估计 NE 浓度为 0.66 nmol/L(95%CI 0.06-1.20 nmol/L)低于刺激前的 NE 浓度。模型模拟表明,处于较高测量丙泊酚浓度(例如 6 mcg/mL)的患者比处于较低测量丙泊酚浓度(例如 3 mcg/mL)的患者表现出更高的 NE 浓度(95%PI 18.10-43.89 nmol/L)(95%PI 16.81-38.91 nmol L)。

结论

具有一阶消除的两室模型可以很好地描述 NE PK。全身麻醉下 NE CL 降低 10%,这种差异归因于测量的丙泊酚浓度。全身麻醉下刺激对 NE PK 的影响非常有限。

临床试验注册号

NL9312。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/225a/11573843/cf8f20f81776/40262_2024_1430_Fig1_HTML.jpg

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