The Cannabinoid CB1/CB2 Agonist WIN55212.2 Promotes Oligodendrocyte Differentiation <i>In Vitro</i> and Neuroprotection During the Cuprizone‐Induced Central Nervous System Demyelination

Tomàs-Roig, Jordi; Wirths, Oliver; Salinas-Riester, Gabriela; Havemann-Reinecke, Ursula

doi:10.1111/cns.12506

Cited by 31 publications

(25 citation statements)

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“…In the prefrontal cortex (PFC), there was an increase in CB receptor 1 binding that coincided with reduced levels of monoacylglycerol lipase, extracellular signal‐regulated kinase, and cyclic adenosine monophosphate response element‐binding protein, which are all critically involved in CB signaling . WIN55 212.2, a CB receptor agonist, increased OPC proliferation in vitro, as well as MBP messenger RNA and protein expression in mice, whereas blocking the metabolism of endogenous CBs decreased OL excitotoxicity and demyelination in vitro, and preserved myelin integrity in a demyelinating mouse model . EtOH exposure alters CB ligands in several brain areas related to memory and addiction (e.g., PFC and amygdala).…”

Section: Etoh Impacts the Development Of Olsmentioning

confidence: 99%

Function and Mechanism of Myelin Regulation in Alcohol Abuse and Alcoholism

Rice

2019

BioEssays

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Excessive alcohol use has adverse effects on the central nervous system (CNS) and can lead to alcohol use disorders (AUDs). Recent studies have suggested that myelin reductions may directly contribute to CNS dysfunctions associated with AUDs. Myelin consists of compact lipid membranes wrapped around axons to provide electrical insulation and trophic support. Regulation of myelin is considered as a new form of neural plasticity due to its profound impacts on the computation of neural networks. In this review, the authors first discuss experimental evidence showing how alcohol exposure causes demyelination in different brain regions, often accompanied by deficits in cognition and emotion. Next, they discuss postulated molecular and cellular mechanisms underlying alcohol's impact on myelin. It is clear that more extensive investigations are needed in this important but underexplored research field in order to gain a better understanding of the myelin-behavior relationship and to develop new treatment strategies for AUDs.

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Section: Etoh Impacts the Development Of Olsmentioning

confidence: 99%

Function and Mechanism of Myelin Regulation in Alcohol Abuse and Alcoholism

Rice

2019

BioEssays

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“…Conversely, histological analysis of the demyelinated area revealed that CNS myelination was slightly compromised when 0.5 mg/Kg of WIN was administered. Similarly, a previous study revealed that the cannabinoid WIN at 0.5 mg/ Kg confers neuroprotection against demyelination while the administration of the drug at 1 mg/Kg aggravates the process 5 . Despite this, it is widely accepted that the cannabinoid receptors modulate the severity of demyelination in distinct experimental animal models 5,32 .…”

Section: Discussionmentioning

confidence: 65%

“…Similarly, a previous study revealed that the cannabinoid WIN at 0.5 mg/ Kg confers neuroprotection against demyelination while the administration of the drug at 1 mg/Kg aggravates the process 5 . Despite this, it is widely accepted that the cannabinoid receptors modulate the severity of demyelination in distinct experimental animal models 5,32 . The administration of CPZ for three weeks led to a pronounced inflammatory reaction by activating the recruitment of microglia and astroglial cells in the demyelinated area 10,33 .…”

Section: Discussionmentioning

confidence: 65%

“…Despite this, several independent groups have demonstrated that the activation of CB 1 receptors in outer mitochondrial membranes regulates respiratory chain complexes and thus, mitochondrial biogenesis (for review see 40 ). Thus, it might be speculate that the drug at 0.5 mg/kg dosage could possess a therapeutic effect probably by protecting neurons against CPZ-induced neurotoxicity through the stimulation of copper-zinc superoxide dismutase enzyme 39 or by promoting the differentiation of oligodendrocytes 5 . On the other hand, 1 mg/kg of the drug had a deleterious effect, presumably related to an inhibitory effect of G i /G o -proteins expressed in neurons as our group postulated on previously 5 .…”

Section: Discussionmentioning

confidence: 99%

“…MS is a chronic inflammatory disorder of the CNS characterized by inflammation and progressive axonal neurites injury terminating in neurodegeneration 2 . The use of the main active component of marijuana, Δ9-tetrahydrocannabinol (THC), has a broad range of therapeutic effects for a variety of medical conditions, including pain, anxiety, glaucoma, and emesis, and also possesses a neuroprotective effect [3][4][5][6] . For our research, we chose the cannabinoid agonist WIN-55,212-2, since this chemical compound has been shown to possess better efficacy at CB 1 -receptor (Ki = 1.9 nM) than THC (Ki = 41 nM) and shows greater binding affinity to CB 1 than CB 2 7,8 .…”

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confidence: 99%

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Dose-dependent effect of cannabinoid WIN-55,212-2 on myelin repair following a demyelinating insult

Tomàs-Roig

Agbemenyah

Celarain

et al. 2020

Sci Rep

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Dysfunctions in the endocannabinoid system have been associated with experimental animal models and multiple sclerosis patients. Interestingly, the endocannabinoid system has been reported to confer neuroprotection against demyelination. The present study aims to assess the effects of the cannabinoid agonist WIN-55,212-2 in cuprizone fed animals on myelin repair capacity. Animals exposed to cuprizone were simultaneously treated withWIN-55,212-2, behaviorally tested and finally the corpus callosum was exhaustively studied by Western blotting, qRT-PCR and a myelin staining procedure. We report that the long-term administration of WIN-55,212-2 reduced the global amount of CB 1 protein. Histological analysis revealed clear demyelination after being fed cuprizone for three weeks. However, cuprizone-fed mice subjected to 0.5 mg/Kg of WIN-55,212-2 displayed no differences when compared to controls during demyelination, although there was a robust increase in the myelinated axons during the remyelination phase. These animals displayed better performance on contextual fear conditioning which was in turn non-attributable to an antinociceptive effect. In contrast, a 1 mg/ Kg dosage caused a remarkable demyelination accompanied by limited potential for myelin repair. Upon drug administration while mice ongoing demyeliniation, the expression of Aif1 (microglia) and Gfap (astrocytes) followed a dose-dependent manner whereas the expression of both markers was apparently attenuated during remyelination. Treatment with vehicle or 0.5 mg/Kg of the drug during demyelination increased the expression of Pdgfra (oligodendrocyte precursor cells) but this did not occur when 1 mg/Kg was administered. In conclusion, the drug at 0.5 mg/Kg did not alter myelin architecture while 1 mg/Kg had a deleterious effect in this model.

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