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In vitro metabolism of cathinone positional isomers: does sex matter?

Research output: Contribution to JournalArticleAcademicpeer-review

Abstract

Synthetic cathinones, one of the most prevalent categories of new psychoactive substances, have been posing a serious threat to public health. Methylmethcathinones (MMCs), notably 3-MMC, have seen an alarming increase in their use in the last decade. The metabolism and toxicology of a large majority of synthetic cathinones, including 3-MMC and 2-MMC, remain unknown. Traditionally, male-derived liver materials have been used as in vitro metabolic incubations to investigate the metabolism of xenobiotics, including MMCs. Therefore, little is known about the metabolism in female-derived in vitro models and the potential sex-specific differences in biotransformation. In this study, the metabolism of 2-MMC, 3-MMC, and 4-MMC was investigated using female rat and human liver microsomal incubations, as well as male rat and human liver microsomal incubations. A total of 25 phase I metabolites of MMCs were detected and tentatively identified using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Seven sex-specific metabolites were detected exclusively using pooled male rat liver microsomal incubations. In addition, the metabolites generated from the sex-dependent in vitro metabolic incubations that were present in both male and female rat liver microsomal incubations showed differences in relative abundance. Yet, neither sex-specific metabolites nor significant differences in relative abundance were observed from pooled human liver microsomal incubations. This is the first study to report the phase I metabolic pathways of MMCs using in vitro metabolic incubations for both male and female liver microsomes, and the relative abundance of the metabolites observed from each sex. Graphical abstract: [Figure not available: see fulltext.].

Original languageEnglish
Pages (from-to)5403-5420
Number of pages18
JournalAnalytical and Bioanalytical Chemistry
Volume415
Issue number22
Early online date15 Jul 2023
DOIs
Publication statusPublished - Sept 2023

Bibliographical note

Funding Information:
Peng Che is funded by a China Scholarship Council (CSC) fellowship (No. 202006210045). Ruben Kranenburg (Amsterdam Dutch Police, The Netherlands) is kindly acknowledged for providing the analytical standards of MMCs. Filip Cuyckens (Janssen R&D, Belgium) and Wilfried Niessen (hyphen MassSpec, the Netherlands) are warmly acknowledged for assisting in MS/MS data interpretation.

Publisher Copyright:
© 2023, The Author(s).

Funding

Peng Che is funded by a China Scholarship Council (CSC) fellowship (No. 202006210045). Ruben Kranenburg (Amsterdam Dutch Police, The Netherlands) is kindly acknowledged for providing the analytical standards of MMCs. Filip Cuyckens (Janssen R&D, Belgium) and Wilfried Niessen (hyphen MassSpec, the Netherlands) are warmly acknowledged for assisting in MS/MS data interpretation. Peng Che is funded by a China Scholarship Council (CSC) fellowship (No. 202006210045). Ruben Kranenburg (Amsterdam Dutch Police, The Netherlands) is kindly acknowledged for providing the analytical standards of MMCs. Filip Cuyckens (Janssen R&D, Belgium) and Wilfried Niessen (hyphen MassSpec, the Netherlands) are warmly acknowledged for assisting in MS/MS data interpretation.

FundersFunder number
MMCs
Wilfried Niessen
China Scholarship Council202006210045

    Keywords

    • In vitro metabolism
    • Methylmethcathinones
    • Positional isomers
    • Sex-specific differences
    • Synthetic cathinones

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