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一种用于测定依托咪酯 Marsh 药代动力学模型“表观 ke0”值的新方法。

A novel technique to determine an 'apparent ke0 ' value for use with the Marsh pharmacokinetic model for propofol.

机构信息

Royal Infirmary of Edinburgh, Edinburgh, UK.

出版信息

Anaesthesia. 2014 May;69(5):420-8. doi: 10.1111/anae.12596.

Abstract

Debate continues over the most appropriate blood-brain equilibration rate constant (ke0) for use with the Marsh pharmacokinetic model for propofol. We aimed to define the optimal ke0 value. Sixty-four patients were sedated with incremental increases in effect-site target concentration of propofol while using six different ke0 values within the range 0.2-1.2 min(-1). Depth of sedation was assessed by measuring visual reaction time. A median 'apparent ke0' value of 0.61 min(-1) (95% CI 0.37-0.78 min(-1)) led to the greatest probability of achieving a stable clinical effect when the effect-site target was fixed at the effect-site concentration displayed by the target-controlled infusion system, at the time when a desired depth of sedation had been reached. By utilising a clinically relevant endpoint to derive this value, inter-individual pharmacokinetic and pharmacodynamic variability may be accounted for.

摘要

关于丙泊酚的 Marsh 药代动力学模型使用的最适血脑平衡速率常数 (ke0),目前仍存在争议。本研究旨在确定最佳的 ke0 值。在使用丙泊酚效应室靶浓度递增的情况下,64 例患者接受镇静治疗,同时在 0.2-1.2 min(-1) 范围内使用了六种不同的 ke0 值。通过测量视觉反应时间评估镇静深度。当效应室靶浓度固定在目标控制输注系统显示的效应室浓度,并且达到所需镇静深度时,中位数“表观 ke0”值为 0.61 min(-1)(95%CI 0.37-0.78 min(-1)),这使得达到稳定临床效果的可能性最大。通过利用临床相关的终点来得出这个值,可以考虑个体间药代动力学和药效学的变异性。

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