4FADB,4F-ADB,: Difference between revisions

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Tremors were observed in mice 30 minutes following 1 mg/kg AMB-FUBINACA in the present study. Pretreatment times and dose ranges for the drug discrimination assay were selected based on the time of peak depression in the locomotor activity assay in mice. Average potency of the discriminative stimulus effects of early compounds was 0.81±0.17 mg/kg (Gatch et al., 2014), whereas the potency of a recent set was 0.09±0.03 mg/kg (Gatch et al., 2018), and the potency of the current set is 0.05±0.01 mg/kg. Short-onset, short-acting compounds have a greater abuse liability, and long-acting compounds pose problems of long-acting adverse effects and interactions with other drugs. The duration of action of the synthetic cannabinoids tested using the 8-h protocol have varied widely, with some producing a duration of action no longer than 1 h, others producing a duration of action between 1–2 h, and others lasting more than 2 h. There seems to be a trend of newer synthetic cannabinoids being more potent than earlier compound

Such decrease remained 2 hr after the administration (Table 4). In locomotor activity, methamphetamine treated group showed approximately 4.2 times increase compared to the negative control treated group. Change of body weight following the treatments with JWH-081 and JWH-210 in mic

These synthetic cannabinoids act 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

All of the compounds tested in the present study depressed locomotor activity as is typical for other synthetic cannabinoids (see review by Wiley et al., 2017). Average horizontal activity counts/10 min as a function of time (10 min bins) and dose. Depressant effects of 1.33 mg/kg were observed within 10 min following administration and peak depressant effects were 5CL ADBA powder observed between 0–30 min. Duration of the locomotor depression increased over dose from 30 min following 0.1 mg/kg to 2.5 h following 1 mg/k

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

4. Drugs
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.
Michael B Gatch
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 5CL ADBA powder highest dose tested (0.5 mg/kg).
Figure 1.
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 mice.
Michael B Gat

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	AMB-FUBINACA ~~has been implicated~~ in ~~severe adverse~~ effects ~~in recreational users~~ (~~Adams~~ et al., ~~2017; Hamilton~~ et al., ~~2017~~), ~~which suggests that~~ the ~~range~~ between ~~behaviorally active~~ and ~~toxic doses~~ of ~~AMB-FUBINACA is narro~~<br><br><br>~~Some mice showed abnormal behaviors (catalepsy, loss of traction, convulsion) right~~ after the administration ~~of the tested substances~~. ~~The~~ locomotor activity ~~of the mice was measured 30 min and~~ 2 ~~hrs after~~ the ~~last substance administration~~. ~~We also examined their neurotoxicity using brain samples through histopathological diagnose, especially in the nucleus accumbens core region. In histopathological analysis, neural cells~~ of the ~~animals treated~~ with ~~the high dose (5 mg/kg) of~~ JWH-081 or JWH-210 ~~showed distorted nuclei and nucleus membranes~~ in ~~the core shell of nucleus accumbens, suggesting neurotoxicity.~~<br>~~Table of Conten~~<br><br>~~<br>Buy Jwh-210~~ at ~~USA K2 INCENSE STORE~~ and ~~enjoy premium quality~~, ~~flexible quantities~~, and ~~fast~~, ~~secure shipping~~. ~~Fast shipping and pure product~~-~~highly recommended for anyone needing quality incense ingredients~~.~~" 🌟🌟🌟🌟🌟 You can buy jwh~~-~~210 online in quantities of 4F~~ ADB ~~10g~~, ~~30g~~, ~~50g~~, ~~100g~~, ~~150g~~, and ~~200g at USA K2 INCENSE STORE for premium quality and discreet shipping. In some areas, it is classified~~ as ~~a controlled substance~~, ~~while~~ in ~~others, it may be legal for research or incense use. The legal status of jwh~~-~~210 varies by country and region.~~<br> ~~Key Features and Specifications to Evaluate~~ <br>~~Higher prices often reflect rigorous quality control rather than markup alone. This compound~~ is ~~appropriate only~~ for ~~authorized professionals conducting lawful research or analysis~~. ~~For legitimate applications~~, ~~only fully characterized, independently tested JWH-210~~ [https://cannabinoidsrc4f-adb.com/ ~~4F ADB~~] ~~should be considered~~.<br> ~~How to Choose Powder JWH-210~~ <br>~~This dual~~-~~use nature underscores the importance~~ of ~~responsible sourcing~~ and ~~strict adherence to legal frameworks~~. ~~Forensic labs~~, ~~public health researchers~~, ~~and customs officials use authentic samples like JWH~~-~~210~~ to ~~distinguish between legal~~ and ~~illegal compounds~~ in ~~seized materials~~. ~~For those seeking a dependable compound for analytical purposes~~, ~~JWH~~-~~210 Chemical Powder provides a trusted~~ and ~~effective solution~~. ~~With its carefully controlled production process~~, ~~stable composition~~, and ~~secure packaging~~, ~~it remains a valuable resource for laboratory~~-~~based researc~~<br><br><br>~~Morris water maze test was performed to evaluate~~ the ~~changes in learning~~ and ~~memory function. Only a few case reports about the dangers of some synthetic cannabinoids due to neurotoxicity~~ have been ~~published~~ (~~Cohen~~ et al., ~~2012; McGuinness et al.~~, ~~2012; Harris~~ and ~~Brown, 2013; Hermanns~~ et al., ~~2013~~). ~~In addition,~~ the ~~lack of information about neurotoxicity of~~ synthetic cannabinoids ~~could allow abusers consume those substances undiscerningly. However, slight structural changes might cause biochemical properties including dependence liability and neurotoxicity. The substances used~~ in the present study ~~both possess naphthoylindole moiety as their parental structure~~. ~~(B) The ratio~~ of ~~damaged cells containing pyknotic or condensed nuclei~~ and ~~low hematoxilin affinity to total cells~~ were ~~calculated~~ in ~~nucleus accumben<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>Due to~~ the ~~unknown toxicity of newly emerging SCRAs~~, ~~forensic assessments of cases involving these substances are challenging. According to the reported cases~~ and ~~reviews of the scientific literature, concurrent ethanol consumption should amplify the toxicity of SCRAs~~. ~~The concentration of 4F~~-~~MDMB-BINACA~~ in the ~~postmortem blood was 2.50 and 2.34 ng/mL~~, and ~~blood alcohol concentration~~ was 2.~~11 and 2~~.~~49 g~~/~~L, respectively. Two fatal cases are reported caused by simultaneous consumption of 4F-MDMB-BINACA and ethanol~~.<br> ~~Fig. 2~~. <br>~~The precursor ion m/z 396~~ (~~B10~~, ~~B12/B15~~) ~~was 32 Da higher than~~ the ~~parent drug~~, 4F-MDMB-~~BINACA~~, ~~suggesting the addition of two hydroxy groups. All the below explanations for transformations into metabolites are based on the data shown in Fig. Metabolites were identified according~~ to ~~their precursor ions~~, ~~product ions, and fragmentation patterns~~ (~~Fig~~. 1). ~~Traditional in-vivo metabolism studies to generate human metabolites~~ of ~~drugs relied heavily on~~ the ~~use of whole animal model systems, which are expensive, limited by drug administration amount, influenced by species variation and faced by many ethical issues. Eight~~ in-~~vivo metabolites tentatively identified were mainly products of ester hydrolysis with or without additional dehydrogenation~~, N-~~dealkylation~~, ~~monohydroxylation and oxidative defluorination with further oxidation to butanoic acid.<br> Fig. 1. <br>Monitoring metabolism of synthetic cannabinoid 4F-~~MDMB-~~BINACA via high~~-~~resolution mass spectrometry assessed in cultured hepatoma cell line, fungus~~, ~~4F ADB liver microsomes~~ and ~~confirmed using urine samples The threshold for fatal overdose of combined use of SCRAs and ethanol can be estimated~~ as ~~a little ng/mL~~ (0.~~37–4~~.~~1 ng/mL according to the reported cases~~) ~~of SCRA and 1.5–2.5 g/L of ethanol. The reported cases and reviews of the scientific literature suggest a possible synergistic effect between SCRAs and ethanol~~, ~~because their combined use clearly increases their toxicity. The victim died due to severe necrotizing pancreatitis and acute kidney injury evolving into multi~~-~~organ failure 11 days after hospital admission . Studies have found no unequivocal synergistic effect between~~ THC ~~and ethanol at low or moderate ethanol doses [29~~, ~~30], but no data on high doses of ethanol are available~~. ~~Given that THC and ethanol act on~~ the ~~same receptors~~, ~~data on their simultaneous use may yield important insights in this regard.<br> Fungus C. elegans <br>Concentrations of 4F-MDMB-BINACA in~~ the ~~postmortem blood samples were 2~~.~~50 and 2.34 ng~~/mL, which ~~are in line with published data. Although the lethal dose of 4F-MDMB-BINACA~~ is ~~unknown, its concentration in postmortem blood samples was found to range between 0.~~10 ~~and 2.90 ng/mL . In SCRA~~-~~related cases in which~~ the ~~deceased suffered from heart disease, the SCRA concentration~~ in the ~~postmortem blood was less than 1 ng/mL~~ . ~~Concentrations of SCRAs in postmortem cases cover a wide range ; however, some reports of survival have also been published—even at relatively high blood SCRA concentrations [19, 20~~		Tremors were observed in mice 30 minutes following 1 mg/kg AMB-FUBINACA in the present study. Pretreatment times and dose ranges for the drug discrimination assay were selected based on the time of peak depression in the locomotor activity assay in mice. Average potency of the discriminative stimulus effects of early compounds was 0.81±0.17 mg/kg (Gatch et al., 2014), whereas the potency of a recent set was 0.09±0.03 mg/kg (Gatch et al., 2018), and the potency of the current set is 0.05±0.01 mg/kg. Short-onset, short-acting compounds have a greater abuse liability, and long-acting compounds pose problems of long-acting adverse effects and interactions with other drugs. The duration of action of the synthetic cannabinoids tested using the 8-h protocol have varied widely, with some producing a duration of action no longer than 1 h, others producing a duration of action between 1–2 h, and others lasting more than 2 h. There seems to be a trend of newer synthetic cannabinoids being more potent than earlier compound<br><br><br>Such decrease remained 2 hr after the administration (Table 4). In locomotor activity, methamphetamine treated group showed approximately 4.2 times increase compared to the negative control treated group. Change of body weight following the treatments with JWH-081 and JWH-210 in mic<br><br><br>These synthetic cannabinoids act 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><br>All of the compounds tested in the present study depressed locomotor activity as is typical for other synthetic cannabinoids (see review by Wiley et al., 2017). Average horizontal activity counts/10 min as a function of time (10 min bins) and dose. Depressant effects of 1.33 mg/kg were observed within 10 min following administration and peak depressant effects were [https://cannabinoidsrc4f-adb.com/ 5CL ADBA powder] observed between 0–30 min. Duration of the locomotor depression increased over dose from 30 min following 0.1 mg/kg to 2.5 h following 1 mg/k<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 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<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 5CL ADBA powder 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 mice.<br>Michael B Gat