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Metabolomics of methadone: clinical and forensic toxicological implications and variability of dose response

机译:美沙酮的代谢组学:临床和法医毒理学意义和剂量反应的变异性

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Methadone is a full -opioid receptor agonist used in the treatment of heroin addiction. It is commercialized as a racemic mixture with considerable variability in the pharmacokinetics and pharmacodynamics between individuals that can affect dose-response and toxicological profile. This review aims to discuss metabolomics of methadone, namely by presenting all major and minor metabolites and pharmacokinetic drug interactions. The main mechanism for methadone metabolism is hepatic through the cytochrome P450, specifically isoenzymes 2B6, 3A4 and 2D6. Firstly, methadone is N-demethylated and cyclize to form its major 2-ethylidene-1,5-dimethyl-3,3-diphenylpyrrolidine (EDDP) and 2-ethyl-5-methyl-3,3-diphenylpyraline (EMDP) metabolites. Several alternate minor pathways have been described namely various methadol metabolites, which proved to be active.It is expected that knowing the metabolomics of methadone may provide further insights, attempting a personalized therapy aiming to attain effective blood concentrations. The historical record is therefore especially important when investigating clinical and forensic cases related to methadone administration, since interindividual responses are known to vary considerably.
机译:美沙酮是一种用于治疗海洛因成瘾的全阿片类受体激动剂。它以消旋混合物形式商业化,在个体之间的药代动力学和药效学中有相当大的差异,会影响剂量反应和毒理学特征。这篇综述旨在讨论美沙酮的代谢组学,即介绍所有主要和次要代谢物以及药代动力学药物相互作用。美沙酮代谢的主要机制是通过细胞色素P450,特别是同工酶2B6、3A4和2D6进入肝脏。首先,将美沙酮进行N-去甲基化并环化以形成其主要的2-亚乙基-1,5-二甲基-3,3-二苯基吡咯烷(EDDP)和2-乙基-5-甲基-3,3-二苯基吡咯啉(EMDP)代谢产物。已经描述了几种替代的次要途径,即各种甲羟吗啡代谢物,它们被证明是有效的。预期了解美沙酮的代谢组学可能会提供进一步的见解,尝试针对个性化疗法以达到有效的血药浓度。因此,在调查与美沙酮给药有关的临床和法医案件时,历史记录尤其重要,因为已知个体间的反应差异很大。

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