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How Do We Use Drug Concentration Data to Improve the Treatment of Overdose Patients?

机译:我们如何使用药物浓度数据来改善药物过量患者的治疗?

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The role of drug assays for screening, diagnosis, and guiding treatment decisions in overdose patients remains unclear. The use of drug concentration data in clinical toxicology research is more problematic, with studies using drug concentrations to simply confirm ingestion in observational studies or others report drug concentration time profiles with simplified pharmacokinetics. The reasons for the lack of more substantial pharmacokinetic and/or pharmacodynamic analysis in overdose patients include problems with uncertainty in dose, uncertainty in the time of ingestion, and limited sampling in the absorption phase. Many of these can be overcome by using population pharmacokinetic and pharmacokinetic-pharmacodynamic analysis in prospective studies of overdose patients to understand dose-concentration-effect relationships. Uncertainty in dose and dose time can be included using population analysis techniques, which may involve a clinical assessment of the veracity of the patient history. The pharmacokinetic-pharmaco-dynamic model can then be used as the basis for predicting toxicity and clinical outcomes from historical information such as dose and early clinical effects. Using such an approach means that the use of drug concentration data in research will improve the risk assessment in overdose patients, without requiring these assays to be rapidly available in the acute health setting.
机译:药物测定在过量患者中筛选,诊断和指导治疗决策的作用尚不清楚。在临床毒理学研究中使用药物浓度数据存在更大的问题,在观察性研究中使用药物浓度简单地确认摄入的研究或其他方法通过简化的药代动力学即可报告药物浓度时间曲线。在用药过量的患者中缺乏更实质的药代动力学和/或药效学分析的原因包括剂量不确定,摄入时间不确定以及吸收阶段采样受限的问题。在过量患者的前瞻性研究中使用群体药代动力学和药代动力学-药效学分析以了解剂量-浓度-效应关系,可以克服许多这些问题。剂量和剂量时间的不确定性可以使用人群分析技术包括在内,这可能涉及对患者病史准确性的临床评估。然后可以将药代动力学-药效学模型用作根据历史信息(例如剂量和早期临床效果)预测毒性和临床结果的基础。使用这种方法意味着在研究中使用药物浓度数据将改善过量患者的风险评估,而无需在急性健康环境中快速进行这些测定。

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