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Translational Antidote Research: A Bedside to Bench Tale

机译:转化解毒剂研究:传奇故事的床头

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Although antidote development should proceed in an orderly fashion from observation, to experimental and safety studies, to clinical trials, this sequence is not always precisely followed. The development of fomepizole as an antidote for toxic alcohol and glycol poisoning is an example of how this may not be the case. Interest in the development of fomepizole was spurred in the 1960s. Shortly thereafter studies characterized by administration to humans commenced. The potential value of fomepizole as an antidote for methanol poisoning was highlighted by primate experiments. Simultaneously, the utility of fomepizole was shown in an experimental model of ethylene glycol poisoning. Further studies on humans showed effectiveness of fomepizole in the treatment of disulfiram-alcohol reactions and ethylene glycol poisoning. In addition, in primate experiments, the safety of fomepizole was established as the subjects tolerated serum fomepizole concentrations over 150 times higher than therapeutic target levels. Subsequent studies have validated the efficacy of fomepizole in the treatment of ethylene glycol and methanol poisonings. Fomepizole has been found to be associated with fewer complications than the alternative alcohol dehydrogenase inhibitor, ethanol. In serious cases of methanol toxicity, fomepizole has been shown to improve survival compared to that obtained with ethanol.
机译:尽管解毒剂的开发应从观察,实验和安全性研究到临床试验以有序的方式进行,但并不总是严格遵循此顺序。氟吡吡唑作为有毒酒精和乙二醇中毒的解毒剂的开发就是可能并非如此的一个例子。在1960年代激起了对Fomepizole研发的兴趣。此后不久,便开始了以对人给药为特征的研究。灵长类动物实验强调了氟吡哌唑作为甲醇中毒的解毒剂的潜在价值。同时,在乙二醇中毒的实验模型中显示了氟吡唑的效用。对人体的进一步研究表明,甲吡咪唑在治疗双硫仑-酒精反应和乙二醇中毒方面有效。此外,在灵长类动物实验中,由于受试者耐受的血清甲吡咪唑浓度比治疗目标水平高150倍以上,因此确定了甲吡咪唑的安全性。随后的研究证实了甲吡咪唑治疗乙二醇和甲醇中毒的疗效。与替代的醇脱氢酶抑制剂乙醇相比,已发现甲吡唑的并发症更少。在严重的甲醇毒性情况下,与使用乙醇相比,已证明吡甲吡唑可提高生存率。

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