In vitro cannabinoid receptor activity, metabolism, and detection in seized samples of CH‐PIATA, a new indole‐3‐acetamide synthetic cannabinoid

Norman, Caitlyn; Deventer, Marie H.; Dremann, Olivia; Reid, Robert; Van Uytfanghe, Katleen; Guillou, Claude; Vinckier, Inge M. J.; Nic Daéid, Niamh; Krotulski, Alex; Stove, Christophe P.

doi:10.1002/dta.3555

Drug Testing and Analysis

2023

DOI: 10.1002/dta.3555

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In vitro cannabinoid receptor activity, metabolism, and detection in seized samples of CH‐PIATA, a new indole‐3‐acetamide synthetic cannabinoid

Caitlyn Norman,

Marie H. Deventer,

Olivia Dremann

et al.

Abstract: The rapidly evolving synthetic cannabinoid receptor agonist (SCRA) market poses significant challenges for forensic scientists. Since the enactment of a generic ban in China, a variety of new compounds have emerged capable of evading the legislation by carrying new structural features. One recent example of a SCRA with new linker and head moieties is CH‐PIATA (CH‐PIACA, CHX‐PIATA, CHX‐PIACA). CH‐PIATA bears an additional methylene spacer in the linker moiety between the indole core and the traditional carbonyl… Show more

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Cited by 2 publications

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In vitro cannabinoid activity profiling of generic ban‐evading brominated synthetic cannabinoid receptor agonists and their analogs

Deventer,

Persson,

Norman

et al. 2023

Drug Testing and Analysis

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Following the enactment of a generic ban in China in 2021, the synthetic cannabinoid market has been evolving, now encompassing even wider structural diversity. Compounds carrying a brominated core such as ADB‐5′Br‐BUTINACA (ADMB‐B‐5Br‐INACA) and tail‐less analogs, such as ADB‐5′Br‐INACA (ADMB‐5Br‐INACA), MDMB‐5′Br‐INACA, and ADB‐INACA (ADMB‐INACA), have been detected since late 2021. This study investigated the cannabinoid receptor (CB) activation potential of synthesized (S)‐enantiomers of these substances, as well as of two predicted analogs MDMB‐5′Br‐BUTINACA (MDMB‐B‐5Br‐INACA) and ADB‐5′F‐BUTINACA (ADMB‐B‐5F‐INACA), using CB1 and CB2 β‐arrestin 2 recruitment assays and a CB1 intracellular calcium release assay. Surprisingly, the tail‐less (S)‐ADB‐5′Br‐INACA and (S)‐MDMB‐5′Br‐INACA retained CB activity, albeit with a decreased potency compared to their tailed counterparts (S)‐ADB‐5′Br‐BUTINACA and (S)‐MDMB‐5′Br‐BUTINACA, respectively, which were potent and efficacious CB1 agonists. Also, at CB2, tail‐less analogs showed a lower potency but increased efficacy. Removing the bromine substitution ((S)‐ADB‐INACA) resulted in a reduced activity at CB1; however, this effect was less prominent at CB2. Looking at tailed analogs, replacing the bromine with a fluorine substitution ((S)‐ADB‐5′F‐BUTINACA) resulted in an increased potency and efficacy at both receptors. Furthermore, as ADB‐5′Br‐INACA and MDMB‐5′Br‐INACA have been frequently detected together in Scottish prisons, this study also evaluated the CB1 receptor activation potential of different mixtures of their respective reference standards, showing no unexpected cannabimimetic effect of combining both substances. Lastly, two powders seized by Belgian Customs and confirmed to contain ADB‐5′Br‐INACA and MDMB‐5′Br‐INACA, respectively, were assessed for CB activity. Based on the comparison with their reference standards, varying degrees of purity were suspected.

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In vitro cannabinoid activity profiling of generic ban‐evading brominated synthetic cannabinoid receptor agonists and their analogs

Deventer,

Persson,

Norman

et al. 2023

Drug Testing and Analysis

Self Cite

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Synthesis, Analytical Characterization, and Human CB1 Receptor Binding Studies of the Chloroindole Analogues of the Synthetic Cannabinoid MDMB-CHMICA

Münster-Müller,

Hansen,

Lucas

et al. 2024

Biomolecules

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Synthetic cannabinoids (SCs) are one of the largest groups of new psychoactive substances (NPSs). However, the relationship between their chemical structure and the affinity to human CB1 receptors (hCB1), which mediates their psychotropic activity, is not well understood. Herein, the synthesis of the 2-, 4-, 5-, 6- and 7-chloroindole analogues of the synthetic cannabimimetic MDMB-CHMICA, along with their analytical characterization via ultraviolet–visible (UV/VIS), infrared (IR), nuclear magnetic resonance (NMR) spectroscopy, and mass spectrometry, is described. Furthermore, all five derivatives of MDMB-CHMICA were analyzed for their hCB1 binding affinities. Chlorination at position 4 and 5 of the indole core reduced the binding affinity compared to MDMB-CHMICA, while the test compounds chlorinated in positions 2, 6, and 7 largely retained their binding affinities relative to the non-chlorinated parent compound.

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In vitro cannabinoid receptor activity, metabolism, and detection in seized samples of CH‐PIATA, a new indole‐3‐acetamide synthetic cannabinoid

Cited by 2 publications

References 48 publications

In vitro cannabinoid activity profiling of generic ban‐evading brominated synthetic cannabinoid receptor agonists and their analogs

In vitro cannabinoid activity profiling of generic ban‐evading brominated synthetic cannabinoid receptor agonists and their analogs

Synthesis, Analytical Characterization, and Human CB1 Receptor Binding Studies of the Chloroindole Analogues of the Synthetic Cannabinoid MDMB-CHMICA

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