Urinary excretion profiles of the orexin receptor antagonist suvorexant and its metabolites.

IF 2.8 4区 医学 Q2 TOXICOLOGY
Misato Wada, Hiroe Kamata, Noriaki Shima, Atsushi Nitta, Hidenao Kakehashi, Shihoko Fujii, Shuntaro Matsuta, Tooru Kamata, Munehiro Katagi, Hiroshi Nishioka
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Abstract

Purpose: Suvorexant is an orexin receptor antagonist used in the treatment of insomnia. In this study, we investigated the urinary excretion profiles of suvorexant and its major metabolites, including conjugates, to obtain fundamental information for proving exposure to suvorexant in criminal cases.

Methods: Urine specimens were collected from three subjects for maximum 168 h after a single oral ingestion of suvorexant (10 mg), and suvorexant and its metabolites in urine were determined using liquid chromatography-tandem mass spectrometry with a C18 semi-micro column.

Results: The carboxylic and hydroxy metabolites (M4 and M9) were identified with authentic standards synthesized in our laboratory, and their glucuronides and other hydroxy metabolites (M8 and M10) were tentatively detected based on measured exact masses and product ion spectra of them. Suvorexant, M4 and M9 would be detectable for 20-34 h, 6-7 days and 42-61 h after intake, respectively. The quantitative results demonstrated that the molar ratios of accumulated amounts of M4 and M9 including their glucuronides excreted in urine to dose ranged about 2.6-6.2% and 0.37-0.51%, respectively, while that of the unchanged parent was much lower (0.011-0.013%). The ratios of the amount of glucuronide to the total amount of M4 and M9 excreted in urine was less than 10% and approximately 90%, respectively.

Conclusions: The urinary excretion profiles indicated that M4 and M9 would be effective indicators for proving suvorexant intake, and M4 could be detected until one week after intake even without enzymatic hydrolysis (limit of detection: 0.05 ng/mL).

食欲素受体拮抗剂suvoexant及其代谢产物的尿排泄谱。
目的:Suvorexant是一种用于治疗失眠的食欲素受体拮抗剂。在这项研究中,我们调查了suvorexant及其主要代谢物(包括偶联物)的尿液排泄情况,以获得证明在刑事案件中暴露于suvorexant的基本信息。方法:采集3名受试者单次口服本品(10 mg)后最长168 h的尿液标本,采用C18半微柱液相色谱-串联质谱法测定尿中本品及其代谢物。结果:用本实验室合成的正品标准品对其中的羧基和羟基代谢物(M4和M9)进行了鉴定,并根据测定的精确质量和产物离子谱初步检测出其中的葡萄糖醛酸酯和其他羟基代谢物(M8和M10)。在摄入后20-34 h、6-7 d和42-61 h可检测到Suvorexant、M4和M9。定量结果表明,M4和M9的累积量(含尿中葡萄糖醛酸酯)与剂量的摩尔比分别为2.6 ~ 6.2%和0.37 ~ 0.51%,而未变化亲本的摩尔比则低得多(0.011 ~ 0.013%)。葡萄糖醛酸苷的量与尿中排出的M4和M9总量的比例分别小于10%和约90%。结论:尿排泄谱提示M4和M9是判定过量摄入的有效指标,且在未酶解的情况下,M4可在摄入后1周检测到(检出限0.05 ng/mL)。
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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来源期刊
Forensic Toxicology
Forensic Toxicology TOXICOLOGY-
CiteScore
5.80
自引率
9.10%
发文量
40
审稿时长
3 months
期刊介绍: The journal Forensic Toxicology provides an international forum for publication of studies on toxic substances, drugs of abuse, doping agents, chemical warfare agents, and their metabolisms and analyses, which are related to laws and ethics. It includes original articles, reviews, mini-reviews, short communications, and case reports. Although a major focus of the journal is on the development or improvement of analytical methods for the above-mentioned chemicals in human matrices, appropriate studies with animal experiments are also published. Forensic Toxicology is the official publication of the Japanese Association of Forensic Toxicology (JAFT) and is the continuation of the Japanese Journal of Forensic Toxicology (ISSN 0915-9606).
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