Substance Details ADB-BUTINACA: Difference between revisions

Revision as of 12:07, 22 May 2026

Figure 1.
Each training session lasted a maximum of 10 min, and the rats could earn up to 20 food pellets. Thirty minutes prior to the training sessions, rats received an injection of either vehicle or Δ9-THC and were subsequently placed in the behavior-testing chambers, where food (45-mg food pellets; Bio-Serve, Frenchtown, NJ) was available as a reinforcer for every ten responses (FR10) on a designated injection appropriate lever. A houselight was centered over the hopper close to the ceiling and was illuminated only when the levers were active. Each dose range included doses that were without effect to those producing at least 50% depression compared to vehicle control. Twenty-four male Sprague-Dawley rats were obtained from Envigo (Houston, TX). Male ND4 Swiss–Webster mice were obtained from Envigo (Houston, TX) at approximately 8 weeks of age and maintained in the University of North Texas Health Science Center (UNTHSC) animal facility for two weeks prior to testin

The current study indicates that the test compounds produce locomotor depression similar to that of Δ9-THC, and fully substitute for the discriminative stimulus effects of Δ9-THC. In summary, these 5F-MDMB-PINACA, MDMB-CHIMICA, MDMB-FUBINACA, ADB-FUBINACA, and AMB-FUBINACA have similar abuse liability as Δ9-tetrahydrocannabinol and should be controlled in a similar fashion. Much of the in vivo 5CL ADBA powder testing of the synthetic cannabinoid compounds have been pre-clinical studies focused on their cannabinoid-like effects or like the present study, focused on their abuse liability. There is indication that at least some of the first-generation synthetic cannabinoids act at receptors other than cannabinoid CB1 and CB2 (Wiley et al., 2016), and a compound from the present study, 5F-MDMB-PINACA, was found to activate midbrain dopamine neurons, but not serotonin neurons (Asaoka et al., 2016

A limitation of this case report is that we did not have a urine sample available for additional NPS testing. Point-of-care DOA tests using urine to screen for misuse of multiple substances, regularly include cannabis, amphetamines, cocaine, opioids, benzodiazepines and methadone. THC, methamphetamine, SRCA, lysergic acid diethylamide (LSD), gamma-hydroxybutyrate (GHB) and ketamine are likely to become volatile under the temperature of current e-cigarettes, while crack cocaine is hard to vaporise. A systematic review including data of 114 patients of which the majority was intoxicated due to SCRA smoking revealed that 45 % of the patients who present at the ER after an intoxication due to SCRA smoking recovered within 24 hours .
Data availability
Moreover, a study conducted in the United Kingdom investigated components of e-liquids in 112 samples originating from prisoners, teenagers and test purchases of commercially available e-cigarettes taken between 2014 and 2021 . This is the first case report that describes the toxicological symptoms of vaping ADB-BUTINACA. Results of the DOA test (including testing for amphetamines, methamphetamines, barbiturates, benzodiazepines, cocaine, methadone, opioids, cannabis, tricyclic antidepressants) were available within 30 minutes and were all negative. We report a case of an involuntary intoxication of the SCRA ADB-BUTINACA after vaping. There are several pitfalls in the detection of SCRA in samples taken from the patient.
Data availabili

In-vitro metabolism studies are generally used to complement these data using perfused organs, tissue or cell cultures and microsomal preparations amongst which pooled human liver microsomes (HLM) have been frequently used to elucidate metabolism of SCBs [12,13,14,15,16

Similarly, precursor ion identified at m/z 380 (B19/B21, B23/B25) was 16 Da higher than the 4F-MDMB-BINACA, indicating monohydroxylation at the butyl side chain (B19/B21) and indazole (B23/B25) moieties with product ions m/z 145 and 161, respectively. Metabolites identified at m/z 366 (B8, B9, B13), which was 16 Da higher than the 4F-MDMB-BINACA ester hydrolysis metabolite (B22), confirmed monohydroxylation upon ester hydrolysis. Death involving these drugs have been reported [5,6,7,8,9], and this raises public health and social concerns. Due to their similar physiological effects to the principal psychoactive component of cannabis, Δ9-tetrahydrocannabinol (THC), SCBs are gaining popularity and are often abused as recreational drugs. The fact that similar 4F-MDMB-BINACA and ethanol concentrations were detected in the postmortem blood samples of both victims suggests that both substances played a role in the fatal outcom

A 30-min period, beginning when maximal depression of locomotor activity first appeared as a function of dose, was used for analysis of dose-response data and calculation of ED50 values. During test sessions, both levers were active, such that ten consecutive responses on either lever led to 5CL ADBA powder reinforcement. The substitution tests occurred only if the rats had achieved 85% injection-appropriate responding on the two prior training sessions.
The locomotor activity assay was used to identify approximate time courses and dose ranges of psychoactive effects, which is useful for identifying parameters for drug discrimination experiments and are also predictive of the time course of the psychoactive effects in human users. The purpose of the present study was to assess the abuse liability of 5F-MDMB-PINACA, MDMB-CHIMICA, MDMB-FUBINACA, ADB-FUBINACA, and AMB-FUBINACA. Since there is currently no robust measure of the reinforcing/rewarding effects of cannabinoids, drug discrimination is currently the best model for assessing abuse liability of cannabinoids. The findings produce an apparent paradox, since CPP and self-administration predict with high reliability the likelihood that a compound will be abused by humans, and cannabinoids are well-known to produce active drug-seeking in human

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	~~These synthetic cannabinoids act [https://cannabinoidsrc4f-adb~~.~~com/ 5CLADBA] directly at cannabinoid CB1~~ and ~~CB2 receptors as does Δ9-tetrahydrocannabinol (~~Δ9-THC~~) found~~ in ~~marijuana~~, ~~but have different chemical structures unrelated to Δ9~~-~~THC~~, ~~different metabolism~~, ~~and often greater toxicity~~ (~~Fantegrossi et al~~.~~, 2014)~~. ~~Discriminative stimulus effects~~ were ~~tested in rats trained~~ to ~~discriminate Δ9~~-~~tetrahydrocannabinol~~ (~~3 mg/kg~~, ~~30-min pretreatment~~). ~~5F-MDMB-PINACA~~ (~~also known as 5F-ADB~~, ~~5F-ADB-PINACA~~)~~, MDMB-CHIMICA, MDMB-FUBINACA, ADB-FUBINACA,~~ and ~~AMB-FUBINACA~~ (~~also known as FUB-AMB, MMB-FUBINACA~~) ~~were tested~~ for ~~in vivo cannabinoid-like effects~~ to ~~assess their abuse liabilit~~<br><br>~~4. Drugs~~ <br>~~In general,~~ the locomotor ~~depressant and discriminative stimulus effects have been observed at doses~~ that ~~do not produce adverse effects, although tremors were observed upon handling in mice that received JWH~~-~~210 (Gatch et al.~~, ~~2016), and 5F-AMB produced sustained vocalization~~ and ~~convulsions in rats (Gatch et al., 2018). All of the synthetic cannabinoids tested in the present study~~ fully ~~substituted~~ for the discriminative stimulus effects of Δ9-THC. ~~Subsequently~~, ~~a one~~-~~way analysis of variance was conducted on horizontal activity counts for the 30~~-~~min period of maximal effect~~, ~~and planned comparisons were conducted for each dose against the vehicle control using single degree~~-of-~~freedom F tests. A two~~-~~way analysis of variance~~, ~~with dose as a between groups factor~~ and time as a within subject factor, was conducted on horizontal activity counts/10 min interval. Locomotor activity in mice was tested to screen for locomotor depressant effects and to identify behaviorally-~~active dose ranges and times of peak effect. Previous studies~~ have ~~demonstrated that these compounds have chemical structures~~ similar ~~to synthetic cannabinoids known to have substantial~~ abuse liability and ~~act at the CB1 receptor~~.~~<br>Michael B Gatch <br>Substantial depressant effects were observed within~~ the ~~first 10 min, and maximal depression was observed between 0–30 min following administration. Tremors were observed 30 minutes following 1 mg/kg AMB-FUBINACA~~ in 3 of ~~8 mice (data not shown). Substantial depressant~~ effects ~~were observed within~~ the ~~first 10 min~~, ~~and maximal depression was observed between 10–40 min and lasted up to 2~~.~~5 to 3 h at the 5CLADBA highest dose tested (0.5 mg/kg).<br>Figure 1. <br>~~There is indication that at least some of the first-generation synthetic cannabinoids act at receptors other than cannabinoid CB1 and CB2 (Wiley et al., 2016), and a compound from the present study, 5F-MDMB-PINACA, was found to activate midbrain dopamine neurons, but not serotonin neurons (Asaoka et al., 2016). ~~As previously mentioned, all~~ of ~~the compounds tested in the present study (MDMB~~-~~PINACA~~, ~~MDMB-CHMICA~~, ~~MDMB-FUBINACA~~, ~~ADB-FUBINACA~~, and ~~AMB-FUBINACA) act as agonists at CB1 receptors (Banister et al~~., ~~2015~~, ~~2016; Gamage et al.~~, ~~2018~~), ~~which suggests these compounds will produce Δ9~~-~~THC~~-~~like effects~~, including ~~abuse liability. Tremors were not observed following AMB-FUBINACA during the drug discrimination study, but~~ the ~~maximum dose tested~~ was ~~only 0.1 mg/kg, which is 10-fold lower than~~ the ~~dose that produced tremors in~~ the ~~mic~~<br><br>~~4. Drugs <br>The purpose of the present~~ study ~~was to assess~~ the ~~abuse liability~~ of 5F-~~MDMB-PINACA~~, ~~MDMB~~-~~CHIMICA, MDMB-FUBINACA, ADB-FUBINACA,~~ and ~~AMB-FUBINACA~~. ~~The findings produce an apparent paradox, since CPP and self-administration predict with high reliability~~ the ~~likelihood~~ that ~~a compound will be abused by humans, and cannabinoids are well-known to produce active drug~~-~~seeking in humans~~. ~~Drug discrimination is a well-known animal model~~ of the ~~subjective effects of drugs and correlates well with abuse liability~~ (~~Young 2009; Horton et al. 2013). Assessment of abuse liability is based on several factors~~, ~~including chemical structure~~, ~~pharmacological mechanism of action~~, ~~and finally~~, ~~subjective and reinforcing behavioral effects (FDA~~, ~~2010; Swedberg~~, ~~2013~~).<br>~~Michael B Gat~~<br><br><br>~~Taken together these data further confirmed the structure elucidation of B16. The~~ precursor ion m/z ~~276~~ (B1) ~~detected, which~~ was 74 Da ~~lower~~ than ~~that for~~ the 4F-MDMB-BINACA ~~ester hydrolysis metabolite~~ (~~B22~~)~~, indicated N-dealkylation of B22. The precursor ion~~ m/z ~~348~~ and ~~product ion detected~~ at m/z ~~217~~ (B2) ~~identified~~ was 2 Da ~~less~~ than the 4F-MDMB-BINACA ester hydrolysis metabolite (B22), ~~indicating oxidative defluorination~~ (~~loss~~ of ~~fluorine with addition of hydroxy 5CLADBA group~~<br><br><br>~~Although there were reports on the metabolism~~ of 4F-~~MDMB-BINACA using in-vivo~~ and ~~various in-vitro models~~, ~~studies~~ were either ~~conducted using small in-vivo sample size such as 1~~ to ~~4 samples~~ [~~5, 29~~] ~~or in closed environments such as forensic psychiatric wards and prisons~~ . The ~~hepatic cell line HepG2 is often used as an initial screen as it is known to produce high reproducibility results with relatively stable enzyme concentration, although they are limited by~~ the ~~low~~-~~level expression of several metabolizing enzymes, including~~ the ~~cytochrome P450 (CYP) class of proteins [17, 18]~~. ~~In-vitro metabolism studies are generally~~ used to ~~complement these data using perfused organs~~, ~~tissue or cell cultures~~ and ~~microsomal preparations amongst which pooled~~ human ~~liver microsomes (HLM) have been frequently used~~ to ~~elucidate metabolism~~ of ~~SCBs [12~~,13,14,15,~~16]~~. Since ~~most SCBs are found extensively in metabolized forms in urine,~~ the ~~identification~~ of ~~metabolites~~ is ~~of vital importance~~ for ~~forensic and clinical toxicologists. Identifying SCB intake and its correlating specific adverse effects require rapid elucidation~~ of ~~these SCBs~~. The ~~proliferation of SCBs has become~~ a ~~global challenge as new compounds~~ are ~~rapidly introduced into the illegal drug market~~ to ~~evade existing~~ drug ~~law~~		Figure 1. <br>Each training session lasted a maximum of 10 min, and the rats could earn up to 20 food pellets. Thirty minutes prior to the training sessions, rats received an injection of either vehicle or Δ9-THC and were subsequently placed in the behavior-testing chambers, where food (45-mg food pellets; Bio-Serve, Frenchtown, NJ) was available as a reinforcer for every ten responses (FR10) on a designated injection appropriate lever. A houselight was centered over the hopper close to the ceiling and was illuminated only when the levers were active. Each dose range included doses that were without effect to those producing at least 50% depression compared to vehicle control. Twenty-four male Sprague-Dawley rats were obtained from Envigo (Houston, TX). Male ND4 Swiss–Webster mice were obtained from Envigo (Houston, TX) at approximately 8 weeks of age and maintained in the University of North Texas Health Science Center (UNTHSC) animal facility for two weeks prior to testin<br><br><br>The current study indicates that the test compounds produce locomotor depression similar to that of Δ9-THC, and fully substitute for the discriminative stimulus effects of Δ9-THC. In summary, these 5F-MDMB-PINACA, MDMB-CHIMICA, MDMB-FUBINACA, ADB-FUBINACA, and AMB-FUBINACA have similar abuse liability as Δ9-tetrahydrocannabinol and should be controlled in a similar fashion. Much of the in vivo 5CL ADBA powder testing of the synthetic cannabinoid compounds have been pre-clinical studies focused on their cannabinoid-like effects or like the present study, focused on their abuse liability. There is indication that at least some of the first-generation synthetic cannabinoids act at receptors other than cannabinoid CB1 and CB2 (Wiley et al., 2016), and a compound from the present study, 5F-MDMB-PINACA, was found to activate midbrain dopamine neurons, but not serotonin neurons (Asaoka et al., 2016<br><br><br>A limitation of this case report is that we did not have a urine sample available for additional NPS testing. Point-of-care DOA tests using urine to screen for misuse of multiple substances, regularly include cannabis, amphetamines, cocaine, opioids, benzodiazepines and methadone. THC, methamphetamine, SRCA, lysergic acid diethylamide (LSD), gamma-hydroxybutyrate (GHB) and ketamine are likely to become volatile under the temperature of current e-cigarettes, while crack cocaine is hard to vaporise. A systematic review including data of 114 patients of which the majority was intoxicated due to SCRA smoking revealed that 45 % of the patients who present at the ER after an intoxication due to SCRA smoking recovered within 24 hours .<br>Data availability <br>Moreover, a study conducted in the United Kingdom investigated components of e-liquids in 112 samples originating from prisoners, teenagers and test purchases of commercially available e-cigarettes taken between 2014 and 2021 . This is the first case report that describes the toxicological symptoms of vaping ADB-BUTINACA. Results of the DOA test (including testing for amphetamines, methamphetamines, barbiturates, benzodiazepines, cocaine, methadone, opioids, cannabis, tricyclic antidepressants) were available within 30 minutes and were all negative. We report a case of an involuntary intoxication of the SCRA ADB-BUTINACA after vaping. There are several pitfalls in the detection of SCRA in samples taken from the patient.<br>Data availabili<br><br>In-vitro metabolism studies are generally used to complement these data using perfused organs, tissue or cell cultures and microsomal preparations amongst which pooled human liver microsomes (HLM) have been frequently used to elucidate metabolism of SCBs [12,13,14,15,16<br><br><br>Similarly, precursor ion identified at m/z 380 (B19/B21, B23/B25) was 16 Da higher than the 4F-MDMB-BINACA, indicating monohydroxylation at the butyl side chain (B19/B21) and indazole (B23/B25) moieties with product ions m/z 145 and 161, respectively. Metabolites identified at m/z 366 (B8, B9, B13), which was 16 Da higher than the 4F-MDMB-BINACA ester hydrolysis metabolite (B22), confirmed monohydroxylation upon ester hydrolysis. Death involving these drugs have been reported [5,6,7,8,9], and this raises public health and social concerns. Due to their similar physiological effects to the principal psychoactive component of cannabis, Δ9-tetrahydrocannabinol (THC), SCBs are gaining popularity and are often abused as recreational drugs. The fact that similar 4F-MDMB-BINACA and ethanol concentrations were detected in the postmortem blood samples of both victims suggests that both substances played a role in the fatal outcom<br><br><br>A 30-min period, beginning when maximal depression of locomotor activity first appeared as a function of dose, was used for analysis of dose-response data and calculation of ED50 values. During test sessions, both levers were active, such that ten consecutive responses on either lever led to [https://cannabinoidsrc4f-adb.com/ 5CL ADBA powder] reinforcement. The substitution tests occurred only if the rats had achieved 85% injection-appropriate responding on the two prior training sessions.<br>The locomotor activity assay was used to identify approximate time courses and dose ranges of psychoactive effects, which is useful for identifying parameters for drug discrimination experiments and are also predictive of the time course of the psychoactive effects in human users. The purpose of the present study was to assess the abuse liability of 5F-MDMB-PINACA, MDMB-CHIMICA, MDMB-FUBINACA, ADB-FUBINACA, and AMB-FUBINACA. Since there is currently no robust measure of the reinforcing/rewarding effects of cannabinoids, drug discrimination is currently the best model for assessing abuse liability of cannabinoids. The findings produce an apparent paradox, since CPP and self-administration predict with high reliability the likelihood that a compound will be abused by humans, and cannabinoids are well-known to produce active drug-seeking in human