Therapeutic Mild Hypothermia and the Pharmacokinetics of Drugs in Trauma Brain Injury (TBI) Patients with a Focus on Sedation, Anticonvulsant and Antibiotic Therapy

F. C. Bagna, S. Pitoni, Peter J D Andrews
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引用次数: 2

Abstract

Background: Therapeutic hypothermia may alter both the pharmacokinetic (PK) and dynamics (PD) of the commonly used drugs in critical care. To achieve maximum benefit, medication dosage and schedules should be optimized. Objective: To review the existing scientific evidence showing the effect of therapeutic hypothermia on the pharmacokinetics of drugs commonly used in the care of patients after Trauma Brain Injury (TBI); particularly including sedatives, anticonvulsants and antibiotics. Data Sources: Computerized searches of OVID MEDLINE, OVID EMBASE, Cochrane Clinical Trials Register to August 2013 and hand searching of references of retrieved articles and proceedings of meetings; associated reference lists; and articles identified by experts in the field. Study Selection: Inclusion criteria were as follows: a) population- humans or animals undergoing therapeutic hypothermia b) design-prospective, randomized controlled trial, c) intervention-hypothermia; measurement of PD and PK of different drugs. Data Extraction: A data extraction form was used and authors (CB & SP) reviewed all trials. Data Synthesis: We reviewed 30 trials that documented changes in PD and PK of sedatives (propofol and midazolam), opioids (fentanyl, remifentanil, alfentil and morphine), anticonvulsants (phenytoin) and antibiotics (aminoglycosides) conducted in human or animal models undergoing therapeutic hypothermia. Conclusion: Data show that therapeutic hypothermia significantly alters the pharmacokinetics of commonly used agents. Particular care should be taken to reduce sedatives once target temperature is reached. Further clinical studies are required to clarify the effect of hypothermia on the PD and PK of therapeutic agents to optimize the benefits of therapeutic hypothermia in the treatment of TBI patients.
以镇静、抗惊厥和抗生素治疗为重点的颅脑损伤(TBI)患者的治疗性亚低温和药物的药代动力学
背景:治疗性低温可能会改变重症监护常用药物的药代动力学(PK)和动力学(PD)。为了达到最大的疗效,应优化用药剂量和用药时间表。目的:综述目前有关治疗性低温对创伤性脑损伤(TBI)患者常用药物药代动力学影响的科学证据;特别是包括镇静剂,抗惊厥药和抗生素。数据来源:计算机检索OVID MEDLINE、OVID EMBASE、Cochrane Clinical Trials Register至2013年8月,手工检索检索到的文献参考文献和会议记录;相关参考书目;以及该领域专家鉴定的文章。研究选择:纳入标准如下:a)人群-接受治疗性低温治疗的人或动物b)设计-前瞻性,随机对照试验c)干预-低温治疗;测定不同药物的PD和PK。数据提取:使用数据提取表,作者(CB & SP)对所有试验进行了回顾。数据综合:我们回顾了30项试验,记录了在接受治疗性低温治疗的人类或动物模型中,镇静剂(异丙酚和咪达唑仑)、阿片类药物(芬太尼、瑞芬太尼、阿芬太尼和吗啡)、抗惊厥药(苯妥英)和抗生素(氨基糖苷类)的PD和PK的变化。结论:数据显示,治疗性低温显著改变了常用药物的药代动力学。一旦达到目标温度,应特别注意减少镇静剂。需要进一步的临床研究来阐明低温治疗对治疗药物PD和PK的影响,以优化治疗性低温治疗TBI患者的益处。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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