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A critical review: does thiopental continuous infusion warrant therapeutic drug monitoring in the critical care population?

机译:严格审查:在重症监护人群中硫喷妥钠持续输注是否需要对治疗药物进行监测?

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Thiopental is a barbiturate used in traumatic brain injuries (TBIs) to reduce intracranial pressure (ICP) and to manage cerebral ischemia. As thiopental follows Michaelis-Menten kinetics, therapeutic drug monitoring (TDM) has been used in practice to improve efficacy and reduce adverse effects. However, its role is still debatable, and TDM is not widely practiced. Current evidence suggests that thiopental therapy may improve mortality and functional outcome in a subpopulation of patients with severe TBI with elevated ICP refractory to conventional medical therapy. Several analytical methods are available to quantify thiopental concentrations. This review uses a previously published 9-step decision-making algorithm to determine whether TDM of thiopental in TBI is warranted. There seems to be poor correlation between thiopental concentration and pharmacological response in terms of neurological response, ICP, electroencephalography, and drug toxicity. There is no established therapeutic range for thiopental continuous infusion due to a wide range of plasma concentrations corresponding to efficacy (25-50 mg/L) and toxicity (30-70 mg/L) and the resulting overlap between the 2. Thiopental exhibits intrapatient and interpatient variability due to age, obesity, renal and hepatic dysfunction, Michaelis-Menten kinetics, and hepatic enzyme autoinduction. Available evidence suggests that TDM of thiopental continuous infusion is not beneficial in improving efficacy or avoiding toxicity. There are however 2 possible scenarios in which TDM may provide additional information to sound clinical judgment. The first is providing patient-specific plasma target concentration to guide titration of therapy. The second scenario is differentiating between brain death and barbiturate-induced coma.
机译:硫喷妥钠是一种巴比妥酸盐,用于颅脑外伤(TBI),以降低颅内压(ICP)和控制脑缺血。由于硫喷妥钠遵循Michaelis-Menten动力学,因此在实践中已使用治疗药物监测(TDM)来提高疗效并减少不良反应。但是,它的作用仍然值得商,,并且TDM并未得到广泛实践。目前的证据表明,硫喷妥钠疗法可改善重度TBI患者亚组的死亡率和功能结局,而传统药物治疗对ICP的抵抗力较差。有几种分析方法可用于量化硫喷妥钠浓度。这项审查使用以前发布的9步骤决策算法来确定是否有必要在TBI中使用硫喷妥特的TDM。就神经反应,ICP,脑电图和药物毒性而言,硫喷妥钠浓度与药理反应之间似乎没有很好的相关性。没有确定的硫喷妥钠连续输注治疗范围,因为对应于功效(25-50 mg / L)和毒性(30-70 mg / L)的广泛血浆浓度以及由此产生的2种之间的重叠。以及由于年龄,肥胖,肾和肝功能障碍,Michaelis-Menten动力学和肝酶自动诱导而引起的患者间差异。现有证据表明,硫喷妥妥钠持续输注的TDM不利于提高疗效或避免毒性。但是,在两种可能的情况下,TDM可能会提供其他信息以进行合理的临床判断。首先是提供患者特定的血浆靶标浓度以指导治疗的滴定。第二种情况是区分脑死亡和巴比妥酸盐引起的昏迷。

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