The cannabinoid ligands SR141716A and AM251 enhance human and mouse islet function via GPR55-independent signalling

Ruz‐Maldonado, Inmaculada; Liu, Bo; Atanes, Patricio; Pingitore, Attilio; Huang, Guo Cai; Choudhary, Pratik; Persaud, Shanta J.

doi:10.1007/s00018-019-03433-6

Cited by 19 publications

(31 citation statements)

References 68 publications

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“…This raises the possibility that GPR55 regulates glucose-stimulated insulin secretion. A recent study found no difference between wildtype and GPR55 knockout mice murine isolated islets of Langerhans in their responses to rimonabant ( Ruz-Maldonado et al, 2020 ), which is consistent with our finding that genotype did not affect the effect of rimonabant on et al glucose homeostasis. The authors did not discuss whether glucose-stimulated insulin secretion differed between islets from wild-type and knockout mice.…”

Section: Discussionsupporting

confidence: 93%

High fat-fed GPR55 null mice display impaired glucose tolerance without concomitant changes in energy balance or insulin sensitivity but are less responsive to the effects of the cannabinoids rimonabant or Δ(9)-tetrahydrocannabivarin on weight gain

Wargent

Kępczyńska

Zaïbi

et al. 2020

PeerJ

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Background The insulin-sensitizing phytocannabinoid, Δ(9)-tetrahydrocannabivarin (THCV) can signal partly via G-protein coupled receptor-55 (GPR55 behaving as either an agonist or an antagonist depending on the assay). The cannabinoid receptor type 1 (CB1R) inverse agonist rimonabant is also a GPR55 agonist under some conditions. Previous studies have shown varied effects of deletion of GPR55 on energy balance and glucose homeostasis in mice. The contribution of signalling via GPR55 to the metabolic effects of THCV and rimonabant has been little studied. Methods In a preliminary experiment, energy balance and glucose homeostasis were studied in GPR55 knockout and wild-type mice fed on both standard chow (to 20 weeks of age) and high fat diets (from 6 to 15 weeks of age). In the main experiment, all mice were fed on the high fat diet (from 6 to 14 weeks of age). In addition to replicating the preliminary experiment, the effects of once daily administration of THCV (15 mg kg−1 po) and rimonabant (10 mg kg−1 po) were compared in the two genotypes. Results There was no effect of genotype on absolute body weight or weight gain, body composition measured by either dual-energy X-ray absorptiometry or Nuclear Magnetic Resonance (NMR), fat pad weights, food intake, energy expenditure, locomotor activity, glucose tolerance or insulin tolerance in mice fed on chow. When the mice were fed a high fat diet, there was again no effect of genotype on these various aspects of energy balance. However, in both experiments, glucose tolerance was worse in the knockout than the wild-type mice. Genotype did not affect insulin tolerance in either experiment. Weight loss in rimonabant- and THCV-treated mice was lower in knockout than in wild-type mice, but surprisingly there was no detectable effect of genotype on the effects of the drugs on any aspect of glucose homeostasis after taking into account the effect of genotype in vehicle-treated mice. Conclusions Our two experiments differ from those reported by others in finding impaired glucose tolerance in GPR55 knockout mice in the absence of any effect on body weight, body composition, locomotor activity or energy expenditure. Nor could we detect any effect of genotype on insulin tolerance, so the possibility that GPR55 regulates glucose-stimulated insulin secretion merits further investigation. By contrast with the genotype effect in untreated mice, we found that THCV and rimonabant reduced weight gain, and this effect was in part mediated by GPR55.

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Section: Discussionsupporting

confidence: 93%

High fat-fed GPR55 null mice display impaired glucose tolerance without concomitant changes in energy balance or insulin sensitivity but are less responsive to the effects of the cannabinoids rimonabant or Δ(9)-tetrahydrocannabivarin on weight gain

Wargent

Kępczyńska

Zaïbi

et al. 2020

PeerJ

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“…As an additional complexity in facing ECS, it has to be taken into account that AM251 exhibits significant activity not only at CB 1 as an inverse agonist/antagonist, but also at orphan cannabinoid G-protein-coupled receptor 55 (GPR55) as an agonist [60][61][62][63]. The lack of homology between cannabinoid receptors may explain the differences among CB 1 and GPR55 in the signaling system and downstream cascade.…”

Section: Discussionmentioning

confidence: 99%

CB1 Activity Drives the Selection of Navigational Strategies: A Behavioral and c-Fos Immunoreactivity Study

Laricchiuta

Balsamo

Fabrizio

et al. 2020

IJMS

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To promote efficient explorative behaviors, subjects adaptively select spatial navigational strategies based on landmarks or a cognitive map. The hippocampus works alone or in conjunction with the dorsal striatum, both representing the neuronal underpinnings of the navigational strategies organized on the basis of different systems of spatial coordinate integration. The high expression of cannabinoid type 1 (CB1) receptors in structures related to spatial learning—such as the hippocampus, dorsal striatum and amygdala—renders the endocannabinoid system a critical target to study the balance between landmark- and cognitive map-based navigational strategies. In the present study, mice treated with the CB1-inverse agonist/antagonist AM251 or vehicle were trained on a Circular Hole Board, a task that could be solved through either navigational strategy. At the end of the behavioral testing, c-Fos immunoreactivity was evaluated in specific nuclei of the hippocampus, dorsal striatum and amygdala. AM251 treatment impaired spatial learning and modified the pattern of the performed navigational strategies as well as the c-Fos immunoreactivity in the hippocampus, dorsal striatum and amygdala. The present findings shed light on the involvement of CB1 receptors as part of the selection system of the navigational strategies implemented to efficiently solve the spatial problem.

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“…In this context, the endocannabinoid system (ECS) is of particular interest since it was targeted by the cannabinoid (CB) receptor type 1 (CB 1 ) antagonist rimonabant to aid weight loss and improve glycaemic control [ 3 , 4 , 5 ]. The ECS is a cell-signaling network formed by endogenous ligands, named endocannabinoids, their enzymes of synthesis and degradation, and their receptors [ 6 , 7 , 8 , 9 ]. Phospholipid-derived endocannabinoids such as 2-arachidonoylglycerol and anandamide act as activators of the canonical CB 1 and CB 2 receptors [ 6 ].…”

Section: Introductionmentioning

confidence: 99%

“…Phospholipid-derived endocannabinoids such as 2-arachidonoylglycerol and anandamide act as activators of the canonical CB 1 and CB 2 receptors [ 6 ]. Both receptors belong to the seven-transmembrane G protein-coupled receptor (GPCR) conserved family and they are distributed centrally and peripherally in active metabolic tissues [ 6 , 9 ].…”

Section: Introductionmentioning

confidence: 99%

“…Several studies have demonstrated that islets express elements of the ECS [ 6 , 8 , 10 , 11 , 12 , 13 , 14 ]. Furthermore, there are reports that cannabinoid receptor ligands can regulate insulin secretion and cell viability [ 9 , 11 , 12 , 13 , 14 , 15 , 16 , 17 ], which are the desired pathways to be enhanced under conditions of impaired glucose tolerance or T2D [ 1 ]. However, a growing number of studies concerning cannabinoid ligand off-target effects highlight the complex pharmacology surrounding the ECS [ 9 , 15 , 18 , 19 ].…”

Section: Introductionmentioning

confidence: 99%

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Direct Stimulatory Effects of the CB2 Ligand JTE 907 in Human and Mouse Islets

Ruz‐Maldonado

Atanes

Huang

et al. 2021

Cells

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Aims: The endocannabinoid system is a complex cell-signaling network through which endogenous cannabinoid ligands regulate cell function by interaction with CB1 and CB2 cannabinoid receptors, and with the novel cannabinoid receptor GPR55. CB1, CB2, and GPR55 are expressed by islet β-cells where they modulate insulin secretion. We have previously shown that administration of the putative CB2 antagonist/inverse agonist JTE 907 to human islets did not affect the insulinotropic actions of CB2 agonists and it unexpectedly stimulated insulin secretion on its own. In this study, we evaluated whether the lack of antagonism could be related to the ability of JTE 907 to act as a GPR55 agonist. Materials and Methods: We used islets isolated from human donors and from Gpr55+/+ and Gpr55−/− mice and quantified the effects of incubation with 10 μM JTE 907 on dynamic insulin secretion, apoptosis, and β-cell proliferation by radioimmunoassay, luminescence caspase 3/7 activity, and immunofluorescence, respectively. We also measured islet IP1 and cAMP accumulation using fluorescence assays, and monitored [Ca2+]i elevations by Fura-2 single cell microfluorometry. Results: JTE 907 significantly stimulated insulin secretion from islets isolated from human donors and islets from Gpr55+/+ and Gpr55−/− mice. These stimulatory effects were accompanied by significant elevations of IP1 and [Ca2+]i, but there were no changes in cAMP generation. JTE 907 also significantly reduced cytokine-induced apoptosis in human and mouse islets and promoted human β-cell proliferation. Conclusion: Our observations show for the first time that JTE 907 acts as a Gq-coupled agonist in islets to stimulate insulin secretion and maintain β-cell mass in a GPR55-independent fashion.

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The cannabinoid ligands SR141716A and AM251 enhance human and mouse islet function via GPR55-independent signalling

Cited by 19 publications

References 68 publications

High fat-fed GPR55 null mice display impaired glucose tolerance without concomitant changes in energy balance or insulin sensitivity but are less responsive to the effects of the cannabinoids rimonabant or Δ(9)-tetrahydrocannabivarin on weight gain

High fat-fed GPR55 null mice display impaired glucose tolerance without concomitant changes in energy balance or insulin sensitivity but are less responsive to the effects of the cannabinoids rimonabant or Δ(9)-tetrahydrocannabivarin on weight gain

CB1 Activity Drives the Selection of Navigational Strategies: A Behavioral and c-Fos Immunoreactivity Study

Direct Stimulatory Effects of the CB2 Ligand JTE 907 in Human and Mouse Islets

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