Characterizing Lomerizine metabolites in camel urine: High-resolution mass spectrometry method development and validation for enhanced doping control

IF 1.8 3区 化学 Q4 BIOCHEMICAL RESEARCH METHODS
Jahfar Nalakath, Rasik Puzhithinipra Thacholil, Ahmed Kadry, Ansar Babu, Ibrahim Waseem, Praseen OK, Christiana Hebel, Narayanan Selvapalam, Erumaipatty Rajagounder Nagarajan
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Abstract

Rationale

Lomerizine (LMZ) is an antimigraine drug that works as a calcium channel blocker and has selective effects on the central nervous system. It is metabolized into trimetazidine (TMZ), which is a prohibited substance owing to its performance-enhancing effects in both human and animal sports. Effective doping control measures are imperative to distinguish the source of TMZ in samples to ensure integrity and fairness of the sport, therefore a comprehensive analysis of LMZ metabolites is essential to identify potential biomarkers in camel urine for effective doping control.

Methods

Camel urine samples were collected from four healthy animals following a single oral administration of LMZ at a dosage of 1 mg/kg body weight. In vitro studies were conducted using homogenized camel liver samples. Lomerizine and its metabolites were extracted using solid-phase extraction and analyzed with a Thermo Fisher Orbitrap Exploris liquid chromatography mass spectrometry system. The acquired data was processed with the Compound Discoverer software.

Results

The study conducted a comprehensive analysis of LMZ metabolites in camels and identified 10 phase I and one phase II metabolites. The primary pathway for the formation of phase I metabolites was de-alkylation, while phase II metabolite was formed through alkylation of the parent drug. The study provided valuable insights into the unique metabolic pathways of LMZ in camels under specific experimental conditions.

Conclusion

The developed method enables the detection and characterization of LMZ and its metabolites in camels. The identified metabolites has the potential to act as marker metabolites for the distinctive detection of LMZ in camel urine to ensure efficient analytical strategies for routine doping control applications.

骆驼尿液中洛美利辛代谢物的特征:为加强兴奋剂控制而进行的高分辨率质谱方法开发和验证。
理由洛美利嗪(LMZ)是一种抗偏头痛药物,是一种钙通道阻滞剂,对中枢神经系统有选择性作用。它被代谢成曲美他嗪 (TMZ),由于曲美他嗪在人类和动物运动中具有提高成绩的作用,因此是一种禁用物质。有效的兴奋剂控制措施必须区分样本中 TMZ 的来源,以确保体育运动的公正性和公平性,因此对 LMZ 代谢物进行全面分析对于确定骆驼尿液中潜在的生物标志物以有效控制兴奋剂至关重要:方法:采集四头健康骆驼的尿样,按每公斤体重 1 毫克的剂量口服 LMZ。使用匀浆骆驼肝脏样本进行了体外研究。采用固相萃取法提取洛美利嗪及其代谢物,并使用 Thermo Fisher Orbitrap Exploris 液相色谱质谱系统进行分析。获得的数据由 Compound Discoverer 软件处理:该研究对骆驼体内的 LMZ 代谢物进行了全面分析,确定了 10 种 I 期代谢物和 1 种 II 期代谢物。I 期代谢物形成的主要途径是去烷基化,而 II 期代谢物则是通过母体药物的烷基化形成的。该研究为了解特定实验条件下骆驼体内 LMZ 的独特代谢途径提供了宝贵的见解:结论:所开发的方法能够检测和鉴定骆驼体内的 LMZ 及其代谢物。鉴定出的代谢物有可能作为标记代谢物,用于骆驼尿液中 LMZ 的独特检测,以确保常规兴奋剂控制应用中的高效分析策略。
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
CiteScore
4.10
自引率
5.00%
发文量
219
审稿时长
2.6 months
期刊介绍: Rapid Communications in Mass Spectrometry is a journal whose aim is the rapid publication of original research results and ideas on all aspects of the science of gas-phase ions; it covers all the associated scientific disciplines. There is no formal limit on paper length ("rapid" is not synonymous with "brief"), but papers should be of a length that is commensurate with the importance and complexity of the results being reported. Contributions may be theoretical or practical in nature; they may deal with methods, techniques and applications, or with the interpretation of results; they may cover any area in science that depends directly on measurements made upon gaseous ions or that is associated with such measurements.
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