Different receptor mechanisms underlying phytocannabinoid‐ versus synthetic cannabinoid‐induced tetrad effects: Opposite roles of CB<sub>1</sub>/CB<sub>2</sub> versus GPR55 receptors

Xiaofei, Wang; Galaj, Ewa; Bi, Guo‐Hua; Zhang, Cindy; He, Yi; Zhan, Jianghua; Bauman, Michael H.; Gardner, Eliot L.; Xi, Zheng‐Xiong

doi:10.1111/bph.14958

Cited by 39 publications

(28 citation statements)

References 53 publications

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“…This effect may be due to the regulation of extracellular dopamine release in the nucleus accumbens (Li et al, 2021). CB 2 -null mice also have a different response to some tetrad tests compared with wild-type mice, particularly the analgesic and catalepsy tests (Liu et al, 2017(Liu et al, , 2020Wang et al, 2020).…”

Section: Implications Of Different Receptor Potenciesmentioning

confidence: 99%

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC

Tagen¹,

Klumpers

2022

British J Pharmacology

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The use of the intoxicating cannabinoid delta-8-tetrahydrocannabinol (Δ 8 -THC) has grown rapidly over the last several years. There have been dozens of Δ 8 -THC studies dating back over many decades, yet no review articles have comprehensively covered these findings. In this review, we summarize the pharmacological studies of Δ 8 -THC, including receptor binding, cell signalling, in vivo cannabimimetic activity, clinical activity and pharmacokinetics. We give special focus to studies that directly compared Δ 8 -THC to its more commonly studied isomer, Δ 9 -THC. Overall, the pharmacokinetics and pharmacodynamics of Δ 8 -THC and Δ 9 -THC are very similar. Δ 8 -THC is a partial agonist of the cannabinoid CB 1 receptor and has cannabimimetic activity in both animals and humans. The reduced potency of Δ 8 -THC in clinical studies compared with Δ 9 -THC can be explained by weaker cannabinoid CB 1 receptor affinity, although there are other plausible mechanisms that may contribute. We highlight the gaps in our knowledge of Δ 8 -THC pharmacology where further studies are needed, particularly in humans.delta-8-THC, pharmacodynamics, pharmacokinetics, Δ 8 -THC | INTRODUCTIONDelta-8-tetrahydrocannabinol (Δ 8 -THC) is a cannabinoid that is a double bond isomer of the more well-known Δ 9 -THC (Figure 1). Δ 8 -THC was first derived from the cyclization of cannabidiol (CBD) and it was discovered to be highly psychoactive in human studies (Adams, 1942).By 1966, it was realized that Δ 8 -THC was present in only negligible amounts in cannabis and cannabis-derived products, such as hash (Hively et al., 1966). Δ 9 -THC was determined to be the compound, almost entirely, responsible for the intoxicating properties of cannabis, including alterations in mood, perception and cognition. Subsequent research focused much more on Δ 9 -THC, but the effects of Δ 8 -THC continued to be characterized throughout the following decades. One reason for this is the better thermodynamic stability of Δ 8 -THC relative to Δ 9 -THC (Hanuš et al., 2016). Note that early studies referred to Δ 8 -THC as Δ 6 or Δ 1(6) and Δ 9 -THC as Δ 1 . This review will follow the modern ring numbering system even when the original publication used the old numbering.There is currently debate about the regulatory status of Δ 8 -THC in the United States (e.g. Koski, 2021). The Agriculture Improvement Act of 2018 (informally called the 'Farm Bill') removed hemp and hemp products containing less than 0.3% Δ 9 -THC from the legal definition of marijuana in the Federal Controlled Substances Act (Agriculture Improvement Act of 2018, 2018). Importantly for Δ 8 -THC, hemp was defined as including 'all derivatives, extracts, cannabinoids, isomers, acids, salts and salts of isomers'. Because Δ 8 -THC is both an isomer of CBD and a derivative of CBD when obtained from the cyclization Abbreviations: C max , maximal concentration; CYP, cytochrome P450; P-gp, P-glycoprotein; Tmax, time to maximal concentration; Δ 8 -THC, delta-8-tetrahydrocannabinol.

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Section: Implications Of Different Receptor Potenciesmentioning

confidence: 99%

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC

Tagen¹,

Klumpers

2022

British J Pharmacology

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“…Effects of THC on temperature appear to mostly be mediated via the CB 1 receptor since the CB 1 antagonist/inverse agonists SR141716 (Rimonabant) and AM-251 have been shown to block effects of cannabinoid agonists such as ∆ 9 -tetrahydrocannabinol (THC) when delivered by parenteral injection (Grim et al, 2017;Taffe et al, 2015) and deletion of the CB 1 receptor in mice prevents hypothermic responses to THC (Wang et al, 2019;Zimmer et al, 1999). Prior studies from this laboratory found that SR141716, administered 15 minutes prior to intraperitoneal injection of THC blocked the body temperature decreases, and tail-flick latency increases (Nguyen et al, 2016b;Taffe et al, 2015;, which is consistent with prior reports that SR141716 pretreatment attenuated a prolactin response to THC (Fernandez-Ruiz et al, 1997) and the hypothermia caused by the CB 1 full agonist WIN 55,212-2 in mice (Son et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

Explication of CB1 receptor contributions to the hypothermic effects of Δ9-tetrahydrocannabinol (THC) when delivered by vapor inhalation or parenteral injection in rats

Nguyen

Creehan

Grant

et al. 2020

Drug and Alcohol Dependence

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The use of ∆ 9 -tetrahydrocannabinol (THC) by inhalation using e-cigarette technology grows increasingly popular for medical and recreational purposes. This has led to development of e-cigarette based techniques to study the delivery of THC by inhalation in laboratory rodents. Inhaled THC reliably produces hypothermic and antinociceptive effects in rats, similar to effects of parenteral injection of THC.This study was conducted to determine the extent to which the hypothermic response depends on interactions with the CB 1 receptor, using pharmacological antagonist (SR141716, AM-251) approaches.Groups of rats were implanted with radiotelemetry devices capable of reporting activity and body temperature, which were assessed after THC inhalation or injection. SR141716 (4 mg/kg, i.p.) blocked or attenuated antinociceptive effects of acute THC inhalation in male and female rats. SR141716 was unable to block the initial hypothermia caused by THC inhalation, but temperature was restored to normal more quickly. Alterations in antagonist pre-treatment time, dose and the use of a rat strain with less sensitivity to THC-induced hypothermia did not change this pattern. Pre-treatment with SR141716 (4 mg/kg, i.p.) blocked hypothermia induced by i.v. THC and reversed hypothermia when administered 45 or 90 minutes after THC (i.p.). SR141716 and AM-251 (4 mg/kg, i.p.) sped recovery from, but did not block, hypothermia caused by vapor THC in female rats made tolerant by prior repeated THC vapor inhalation. The CB 2 antagonist AM-630, had no effect. These results suggest that hypothermia consequent to THC inhalation is induced by other mechanisms in addition to CB 1 receptor activation.

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“…The open field test (OFT) was performed to determine whether Mepirapim treatment induces hypomotility. The test used previously reported experimental designs, with minor modifications [36]. The open field was an opaque plastic box (30 × 30 × 30 cm), divided into 16 (4 × 4) equal sectors (7.5 × 7.5 cm).…”

Section: Open Field Testmentioning

confidence: 99%

“…Body temperature ( • C) measurements were taken, with minor modifications of previously reported experimental designs, to determine whether Mepirapim treatment induces hypothermia [36]. After the basal body temperature was measured, mice were treated with the drug.…”

Section: Body Temperature Measurementmentioning

confidence: 99%

Mepirapim, a Novel Synthetic Cannabinoid, Induces Addiction-Related Behaviors through Neurochemical Maladaptation in the Brain of Rodents

et al. 2022

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Mepirapim is a synthetic cannabinoid that has recently been abused for recreational purposes. Although serious side effects have been reported from users, the dangerous pharmacological effects of Mepirapim have not been scientifically demonstrated. In this study, we investigated the addictive potential of Mepirapim through an intravenous self-administration test and a conditioned place preference test in rodents. Moreover, to determine whether the pharmacological effects of Mepirapim are mediated by cannabinoid receptors, we investigated whether Mepirapim treatment induces cannabinoid tetrad symptoms in mice. Lastly, to identify Mepirapim induced neurochemical maladaptation in the brains of mice, we performed microdialysis, western blots and neurotransmitter enzyme-linked immunosorbent assays. In the results, Mepirapim supported the maintenance of intravenous self-administration and the development of conditioned place preference. As a molecular mechanism of Mepirapim addiction, we identified a decrease in GABAeric signalling and an increase in dopaminergic signalling in the brain reward circuit. Finally, by confirming the Mepirapim-induced expression of cannabinoid tetrad symptoms, we confirmed that Mepirapim acts pharmacologically through cannabinoid receptor one. Taken together, we found that Mepirapim induces addiction-related behaviours through neurochemical maladaptation in the brain. On the basis of these findings, we propose the strict regulation of recreational abuse of Mepirapim.

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Different receptor mechanisms underlying phytocannabinoid‐ versus synthetic cannabinoid‐induced tetrad effects: Opposite roles of CB₁/CB₂ versus GPR55 receptors

Cited by 39 publications

References 53 publications

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC

Explication of CB1 receptor contributions to the hypothermic effects of Δ9-tetrahydrocannabinol (THC) when delivered by vapor inhalation or parenteral injection in rats

Mepirapim, a Novel Synthetic Cannabinoid, Induces Addiction-Related Behaviors through Neurochemical Maladaptation in the Brain of Rodents

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Different receptor mechanisms underlying phytocannabinoid‐ versus synthetic cannabinoid‐induced tetrad effects: Opposite roles of CB1/CB2 versus GPR55 receptors

Cited by 39 publications

References 53 publications

Review of delta‐8‐tetrahydrocannabinol (Δ8‐THC): Comparative pharmacology with Δ9‐THC

Review of delta‐8‐tetrahydrocannabinol (Δ8‐THC): Comparative pharmacology with Δ9‐THC

Explication of CB1 receptor contributions to the hypothermic effects of Δ9-tetrahydrocannabinol (THC) when delivered by vapor inhalation or parenteral injection in rats

Mepirapim, a Novel Synthetic Cannabinoid, Induces Addiction-Related Behaviors through Neurochemical Maladaptation in the Brain of Rodents

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Different receptor mechanisms underlying phytocannabinoid‐ versus synthetic cannabinoid‐induced tetrad effects: Opposite roles of CB₁/CB₂ versus GPR55 receptors

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC

Review of delta‐8‐tetrahydrocannabinol (Δ⁸‐THC): Comparative pharmacology with Δ⁹‐THC