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将治疗干预措施纳入乙二醇意外或故意过量服用的人体临床病例报告的生理药代动力学模型中。

Incorporation of therapeutic interventions in physiologically based pharmacokinetic modeling of human clinical case reports of accidental or intentional overdosing with ethylene glycol.

作者信息

Corley R A, McMartin K E

机构信息

Battelle Pacific Northwest Division, Richland, Washington 99352, USA.

出版信息

Toxicol Sci. 2005 May;85(1):491-501. doi: 10.1093/toxsci/kfi120. Epub 2005 Feb 16.

DOI:10.1093/toxsci/kfi120
PMID:15716481
Abstract

Although occupational uses of the high production volume (HPV) chemical ethylene glycol (EG) have not been associated with adverse effects, there are case reports where humans have either intentionally or accidentally ingested large quantities of EG, primarily from antifreeze. The acute toxicity of EG can proceed through three stages, each associated with a different metabolite: central nervous system depression (ethylene glycol), cardiopulmonary effects associated with metabolic acidosis (glycolic acid), and ultimately renal toxicity (oxalic acid), depending on the total amounts consumed and the effectiveness of therapeutic interventions. A physiologically based pharmacokinetic (PBPK) model developed in a companion paper (Corley et al., 2005). Development of a physiologically based pharmacokinetic model for ethylene glycol and its metabolite, glycolic acid, in rats and humans. Toxicol. Sci., in press 2005) was refined in this study to include clinically relevant treatment regimens for EG poisoning such as hemodialysis or metabolic inhibition with either ethanol or fomepizole. Such modifications enabled the model to describe data from several human case reports, confirming the ability of the previous model to describe the pharmacokinetics of EG and its metabolite, glycolic acid, in humans across a broad range of doses and multiple exposure routes. By integrating the case report data sets with controlled studies in this PBPK model, it was demonstrated that fomepizole, if administered early enough in a clinical situation, can be more effective than ethanol or hemodialysis in preventing the metabolism of EG to more toxic metabolites. Hemodialysis remains an important option, however, if treatment is instituted after a significant amount of EG is metabolized or if renal toxicity has occurred.

摘要

尽管高产量(HPV)化学品乙二醇(EG)的职业用途未显示出不良反应,但有病例报告称人类有意或意外摄入了大量EG,主要来自防冻液。EG的急性毒性可经历三个阶段,每个阶段与不同的代谢产物相关:中枢神经系统抑制(乙二醇)、与代谢性酸中毒相关的心肺效应(乙醇酸),以及最终的肾毒性(草酸),这取决于摄入总量和治疗干预的效果。在一篇配套论文(Corley等人,2005年。《乙二醇及其代谢产物乙醇酸在大鼠和人类中的基于生理的药代动力学模型的开发》。《毒理学科学》,即将发表,2005年)中开发的基于生理的药代动力学(PBPK)模型在本研究中得到了完善,以纳入针对EG中毒的临床相关治疗方案,如血液透析或用乙醇或甲吡唑进行代谢抑制。这些修改使该模型能够描述来自几例人类病例报告的数据,证实了先前模型在广泛剂量和多种暴露途径下描述EG及其代谢产物乙醇酸在人体内药代动力学的能力。通过将病例报告数据集与该PBPK模型中的对照研究相结合,结果表明,在临床情况下,如果甲吡唑给药足够早,在预防EG代谢为毒性更强的代谢产物方面可能比乙醇或血液透析更有效。然而,如果在大量EG代谢后才开始治疗或已经发生肾毒性,血液透析仍然是一个重要的选择。

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