Exploring Stereochemical and Conformational Requirements at Cannabinoid Receptors for Synthetic Cannabinoids Related to SDB-006, 5F-SDB-006, CUMYL-PICA, and 5F-CUMYL-PICA

Ametovski, Adam; Macdonald, Courtney; Manning, Jamie J.; Haneef, S. A. Syed; Santiago, Marina; Martin, L.; Sparkes, Eric; Reckers, Andrew; Gerona, Roy; Connor, Mark; Glass, Michelle; Banister, Samuel D.

doi:10.1021/acschemneuro.0c00591

Cited by 15 publications

(26 citation statements)

References 55 publications

(134 reference statements)

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“…Antonides et al [31] analysed sized herbal products, reporting a predominance of the (S)-enantiomer of AMB-FUBINACA in all samples (96.8 to 98.2%), which is in line with studies revealing the (S)-enantiomer of other SCs as the most prevalent or the only detected in illicit herbal products [30]]. Of note, the (S)-enantiomer is generally more potent than the (R)-enantiomer in both CB1R and CB2R [30,32,34], the potency varying amongst SCs [31,33]. In this line, (S)-AMB-FUBINACA has greater ADB-FUBINACA is the methylated analogue of the SC AB-FUBINACA (Figure 1), which was also developed and patented (patent reference: WO 2009/106980-A2) by Ingrid Buchler and her colleagues at Pfizer Inc. in 2009, having never been tested in humans [8,29].…”

Section: Chemistry and Chemical Analysissupporting

confidence: 87%

“…The potency in the (R)-enantiomer increases for SCs displaying the configuration of valinate methyl ester, at the detriment of valinamide, leucinamide or tert-leucine methyl ester. In addition, the efficacy of the (S)-AMB-FUBINACA was also found to be almost two times greater in CB1R, with a maximal response (E max ) of 267% for the (S)-enantiomer and 154% for the (R)-enantiomer, as compared to the control (JWH-018); while the efficacy in CB2R was lower for the (S)-enantiomer (E max of 161%), when compared to the (R)-enantiomer (E max of 205%) [31,33,34].…”

Section: Chemistry and Chemical Analysismentioning

confidence: 95%

“…AMB-FUBINACA has also the (S)-and (R)-configurations and the chiral centre at the C-2 carbon of the valinate side chain [29]. Chirality is common among SCs, implying different pharmacological and toxicological potencies among enantiomers [30][31][32][33][34]. As such, the assessment of the proportions of (S)-and (R)-enantiomers in the seized materials may allow for a better estimate of the risks users are exposed to.…”

Section: Chemistry and Chemical Analysismentioning

confidence: 99%

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Overview of Synthetic Cannabinoids ADB-FUBINACA and AMB-FUBINACA: Clinical, Analytical, and Forensic Implications

et al. 2021

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ADB-FUBINACA and AMB-FUBINACA are two synthetic indazole-derived cannabinoid receptor agonists, up to 140- and 85-fold more potent, respectively, than trans-∆9-tetrahydrocannabinol (∆9-THC), the main psychoactive compound of cannabis. Synthesised in 2009 as a pharmaceutical drug candidate, the recreational use of ADB-FUBINACA was first reported in 2013 in Japan, with fatal cases being described in 2015. ADB-FUBINACA is one of the most apprehended and consumed synthetic cannabinoid (SC), following AMB-FUBINACA, which emerged in 2014 as a drug of abuse and has since been responsible for several intoxication and death outbreaks. Here, we critically review the physicochemical properties, detection methods, prevalence, biological effects, pharmacodynamics and pharmacokinetics of both drugs. When smoked, these SCs produce almost immediate effects (about 10 to 15 s after use) that last up to 60 min. They are rapidly and extensively metabolised, being the O-demethylated metabolite of AMB-FUBINACA, 2-(1-(4-fluorobenzyl)-1H-indazole-3-carboxamide)-3-methylbutanoic acid, the main excreted in urine, while for ADB-FUBINACA the main biomarkers are the hydroxdimethylpropyl ADB-FUBINACA, hydroxydehydrodimethylpropyl ADB-FUBINACA and hydroxylindazole ADB-FUBINACA. ADB-FUBINACA and AMB-FUBINACA display full agonism of the CB1 receptor, this being responsible for their cardiovascular and neurological effects (e.g., altered perception, agitation, anxiety, paranoia, hallucinations, loss of consciousness and memory, chest pain, hypertension, tachycardia, seizures). This review highlights the urgent requirement for additional studies on the toxicokinetic properties of AMB-FUBINACA and ADB-FUBINACA, as this is imperative to improve the methods for detecting and quantifying these drugs and to determine the best exposure markers in the various biological matrices. Furthermore, it stresses the need for clinicians and pathologists involved in the management of these intoxications to describe their findings in the scientific literature, thus assisting in the risk assessment and treatment of the harmful effects of these drugs in future medical and forensic investigations.

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Section: Chemistry and Chemical Analysissupporting

confidence: 87%

Section: Chemistry and Chemical Analysismentioning

confidence: 95%

Section: Chemistry and Chemical Analysismentioning

confidence: 99%

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Overview of Synthetic Cannabinoids ADB-FUBINACA and AMB-FUBINACA: Clinical, Analytical, and Forensic Implications

et al. 2021

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“…Halogenated JWH-018 was less effective in causing seizures, myoclonia, and hyperreflexia than JWH-018 [ 83 ]. Moreover, the enantiomeric configuration might have a role in the affinity to receptors [ 84 , 85 ].…”

Section: Resultsmentioning

confidence: 99%

“…Harmful effects of NPS have been repeatedly proven to be fatal as reported by case reports, case series, and reviews present in the literature [ 7 , 85 , 165 , 166 , 167 , 168 ]. Also, data from studies applied to animals, conducted so far mostly in mice, unequivocally draw great attention to the acute toxic effects of these chemicals [ 169 , 170 , 171 ].…”

Section: Discussionmentioning

confidence: 99%

Molecular Mechanisms of Action of Novel Psychoactive Substances (NPS). A New Threat for Young Drug Users with Forensic-Toxicological Implications

Giorgetti

Pascali

Fais

et al. 2021

Life

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Novel psychoactive substances (NPS) represent a severe health risk for drug users. Even though the phenomenon has been growing since the early 2000s, the mechanisms of action of NPS at the receptors and beyond them are still scarcely understood. The aim of the present study was to provide a systematic review of the updated knowledge regarding the molecular mechanisms underlying the toxicity of synthetic opioids, cannabinoids, cathinones, and stimulants. The study was conducted on the PubMed database. Study eligibility criteria included relevance to the topic, English language, and time of publication (2010–2020). A combined Mesh and free-text protocols search was performed. Study selection was performed on the title/abstract and, in doubtful cases, on the full texts of papers. Of the 580 records identified through PubMed searching and reference checking, 307 were excluded by title/abstract and 78 additional papers were excluded after full-text reading, leaving a total of 155 included papers. Molecular mechanisms of synthetic opioids, synthetic cannabinoids, stimulants, psychedelics, and hallucinogens were reviewed and mostly involved both a receptor-mediated and non-receptor mediated cellular modulation with multiple neurotransmitters interactions. The molecular mechanisms underlying the action of NPS are more complex than expected, with a wide range of overlap among activated receptors and neurotransmitter systems. The peculiar action profile of single compounds does not necessarily reflect that of the structural class to which they belong, accounting for possible unexpected toxic reactions.

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Redox cascade reaction for kinetic resolution of racemic α-methylbenzylamine and biosynthesis of α-phenylethanol

Wang

Chen

Deng

et al. 2022

Appl Microbiol Biotechnol

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Exploring Stereochemical and Conformational Requirements at Cannabinoid Receptors for Synthetic Cannabinoids Related to SDB-006, 5F-SDB-006, CUMYL-PICA, and 5F-CUMYL-PICA

Cited by 15 publications

References 55 publications

Overview of Synthetic Cannabinoids ADB-FUBINACA and AMB-FUBINACA: Clinical, Analytical, and Forensic Implications

Overview of Synthetic Cannabinoids ADB-FUBINACA and AMB-FUBINACA: Clinical, Analytical, and Forensic Implications

Molecular Mechanisms of Action of Novel Psychoactive Substances (NPS). A New Threat for Young Drug Users with Forensic-Toxicological Implications

Redox cascade reaction for kinetic resolution of racemic α-methylbenzylamine and biosynthesis of α-phenylethanol

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