3-CMC, 4-CMC, and 4-BMC Human Metabolic Profiling: New Major Pathways to Document Consumption of Methcathinone Analogues?-Reference-Cited by-同舟云学术

3-CMC, 4-CMC, and 4-BMC Human Metabolic Profiling: New Major Pathways to Document Consumption of Methcathinone Analogues?

Published:2024-06-11 Issue:4 Volume:26 Page:
ISSN:1550-7416
Container-title:The AAPS Journal
language:en
Short-container-title:AAPS J

Author:

Berardinelli Diletta,Taoussi Omayema,Daziani Gloria,Tavoletta Francesco,Ricci Giovanna,Tronconi Livio P.,Adamowicz Piotr,Busardò Francesco P.^ORCID,Carlier Jeremy

Abstract

Abstract Synthetic cathinones represent one of the largest and most abused new psychoactive substance classes, and have been involved in numerous intoxications and fatalities worldwide. Methcathinone analogues like 3-methylmethcathinone (3-MMC), 3-chloromethcathinone (3-CMC), and 4-CMC currently constitute most of synthetic cathinone seizures in Europe. Documenting their consumption in clinical/forensic casework is therefore essential to tackle this trend. Targeting metabolite markers is a go-to to document consumption in analytical toxicology, and metabolite profiling is crucial to support investigations. We sought to identify 3-CMC, 4-CMC, and 4-bromomethcathinone (4-BMC) human metabolites. The substances were incubated with human hepatocytes; incubates were screened by liquid chromatography-high-resolution tandem mass spectrometry and data were mined with Compound Discoverer (Themo Scientific). 3-CMC-positive blood, urine, and oral fluid and 4-CMC-positive urine and saliva from clinical/forensic casework were analyzed. Analyses were supported by metabolite predictions with GLORYx freeware. Twelve, ten, and ten metabolites were identified for 3-CMC, 4-CMC, and 4-BMC, respectively, with similar transformations occurring for the three cathinones. Major reactions included ketoreduction and N-demethylation. Surprisingly, predominant metabolites were produced by combination of N-demethylation and ω-carboxylation (main metabolite in 3-CMC-positive urine), and combination of β-ketoreduction, oxidative deamination, and O-glucuronidation (main metabolite in 4-CMC-positive urine). These latter metabolites were detected in negative-ionization mode only and their non-conjugated form was not detected after glucuronide hydrolysis; this metabolic pathway was never reported for any methcathinone analogue susceptible to undergo the same transformations. These results support the need for comprehensive screening strategies in metabolite identification studies, to avoid overlooking significant metabolites and major markers of consumption. Graphical Abstract

Funder

Università Politecnica delle Marche

Publisher

Springer Science and Business Media LLC

Link

https://link.springer.com/content/pdf/10.1208/s12248-024-00940-8.pdf

Reference30 articles.

1. Daziani G, Lo Faro AF, Montana V, Goteri G, Pesaresi M, Bambagiotti G, et al. Synthetic cathinones and neurotoxicity risks: a systematic review. Int J Mol Sci. 2023;24:6230. https://doi.org/10.3390/ijms24076230.

2. European Monitoring Centre for Drugs and Drug Addiction. European Drug Report 2023: Trends and Developments 2024. https://www.emcdda.europa.eu/publications/european-drug-report/2023_en. Accessed 25 Mar 2024.

3. Carlier J, Berardinelli D, Montanari E, Sirignano A, Di Trana A, Busardò FP. 3F-α-pyrrolydinovalerophenone (3F-α-PVP) in vitro human metabolism: multiple in silico predictions to assist in LC-HRMS/MS analysis and targeted/untargeted data mining. J Chromatogr B. 2022;1193:123162. https://doi.org/10.1016/j.jchromb.2022.123162.

4. Nadal-Gratacós N, Lleixà E, Gibert-Serramià M, Estrada-Tejedor R, Berzosa X, Batllori X, et al. Neuropsychopharmacology of emerging drugs of abuse: Meta- and Para-halogen-ring-substituted α-PVP (“flakka”) derivatives. Int J Mol Sci. 2022;23:2226. https://doi.org/10.3390/ijms23042226.

5. Lopes RP, Ferro RA, Milhazes M, Figueira M, Caldeira MJ, Antunes AMM, et al. Metabolic stability and metabolite profiling of emerging synthetic cathinones. Front Pharmacol. 2023;14:1–14. https://doi.org/10.3389/fphar.2023.1145140.