Endocannabinoid System and Exogenous Cannabinoids in Depression and Anxiety: A Review.

paper Cited Public

Authors: Hasbi, Ahmed; Madras, Bertha K; George, Susan R
Year: 2023
Journal: Brain sciences
PMID: 36831868
DOI: 10.3390/brainsci13020325
PMCID: PMC9953886

Figure 1

Schematic representation of the endocannabinoid signaling system. Endocannabinoids (eCBs) 2AG (2-arachidonoylglycerol) and AEA (anandamide) are synthesized in postsynaptic neurons and act pre-synaptically at their receptors (CB1Rs) in a retrograde mode (A). eCBs can also activate CB1R localized post-synaptically in some cases. In general, activation of CB1 receptors by eCBs decreases the probability of neurotransmitter release through multiple mechanisms, comprising inhibition of calcium influx and activation of potassium channels These effects are terminated by eCB reuptake followed by degradation: 2AG by MAGL pre-synaptically and AEA by FAAH post-synaptically. A large proportion (45–48%) of synapses in different brain regions is tripartite (B), formed by pre-synaptic and post-synaptic neurons, and a glial cell—an astrocyte—which expresses CB1R. In response to neuronal activation, eCBs released by the postsynaptic neurons can activate CB1R expressed on astrocytes. The astrocytes respond with an increase in intracellular calcium leading to release of gliotransmitters (B).

LLM interpretation

This figure is a schematic diagram illustrating the endocannabinoid signaling system in two scenarios: (A) a bipartite synapse and (B) a tripartite synapse involving an astrocyte. The diagrams show the synthesis of 2-AG and AEA in the postsynaptic neuron, their retrograde transport to activate pre-synaptic CB1 receptors (CB1R) to inhibit neurotransmitter release, and their subsequent degradation by MAGL and FAAH. Panel B further depicts eCBs activating CB1R on an astrocyte, triggering an increase in intracellular calcium ($\text{Ca}^{2+}$) and the release of gliotransmitters.

Figure 2

Modulation of neuronal activity by the endocannabinoid system. Endocannabinoids modulate neuronal activity as illustrated for dopamine (DA) neurons with cell bodies in the ventral tegmental area (VTA). CB1 receptors on GABAergic terminals (A) can facilitate dopaminergic activity through suppression of the inhibitory input onto the GABA receptors present on DA neurons, leading to an increase of DA release. Further, the activation of mGluR5 receptor by released glutamate (B) leads to the synthesis and release of 2-arachidonoylglycerol (2-AG), which then retrogradely activates CB1 receptors to inhibit additional glutamate release.

LLM interpretation

This figure is a schematic diagram illustrating the modulation of dopamine (DA) neurons in the ventral tegmental area (VTA) by the endocannabinoid system. Panel A shows how 2-AG activates CB1 receptors on GABAergic terminals to suppress inhibitory input, resulting in increased DA release at the nucleus accumbens (NAc) terminal. Panel B depicts a retrograde signaling pathway where glutamate activates mGluR5 receptors, triggering the synthesis of 2-AG via PLC and DAGL to inhibit further glutamate release through CB1 receptors.

#	Section	Preview
0	1. Introduction	There is evidence that humans have used Cannabis sativa since ancient times for recreational and/or…
1	1. Introduction	The purpose of this mini-review is to explore the association between depression or anxiety and the…
2	1. Introduction	We describe the most important constituents of Cannabis sativa, review the endocannabinoid system,…
3	2. Constituents of Cannabis sativa	The chemical nature of the constituents of Cannabis sativa is diverse, with the number of natural…
4	3. Cannabinoid Receptors	Two receptors have been identified as the main cannabinoid receptors, the CB1 and CB2 receptors. The…
5	4. Additional Receptors for Cannabinoids	Beside their actions through the CB1 and CB2 receptors, the endocannabinoids, as well as the…
6	5. The Endocannabinoid System	The endocannabinoid system (ECS) consists of the cannabinoid receptors, the endogenous cannabinoids…
7	5. The Endocannabinoid System — 5.1. Endocannabinoids	The primary eCBs are anandamide (AEA) and 2-arachidonoylglycerol (2-AG) (reviewed in [5]).…
8	5. The Endocannabinoid System — 5.2. Enzymes Responsible for the Synthesis and Degradation of eCBs	Endocannabinoids are lipophilic molecules synthesized ‘on demand’, meaning synthesis occurs…
9	6. Signaling of the ECS	The mode of action of the eCBs on their receptors (Figure 1) reveals that eCBs synthesized in…
10	6. Signaling of the ECS	neurons and activate CB1R expressed on astrocytes. The astrocytes respond with an increase in…
11	6. Signaling of the ECS	In contrast, CB1 receptors at glutamatergic synapses, suppress excitatory inputs onto the…
12	7. Reuptake of eCBs	It has been suggested that eCBs are removed from the synaptic space by an uptake mechanism followed…
13	8. Cannabinoids in Depression and Anxiety	Because depression and anxiety commonly accompany multiple other disorders, their etiology can be…
14	8. Cannabinoids in Depression and Anxiety — 8.1. Cannabinoids and Depression-like Effects in Animal Studies	In preclinical studies using animal model systems, mostly in rodents, cannabinoids, whether…
15	8. Cannabinoids in Depression and Anxiety — 8.1. Cannabinoids and Depression-like Effects in Animal Studies	There are a few animal tests used to investigate depression-like and anxiety-like behaviors, such as…
16	8. Cannabinoids in Depression and Anxiety — 8.1. Cannabinoids and Depression-like Effects in Animal Studies	Several lines of evidence suggest that acute enhancement of CB1R activity results in antidepressant-…
17	8. Cannabinoids in Depression and Anxiety — 8.2. Evidence for the Involvement of the ECS in Depression, Anxiety, and Stress	The involvement of the CB1R in the above-described effects of cannabinoids was usually verified by…
18	8. Cannabinoids in Depression and Anxiety — 8.2. Evidence for the Involvement of the ECS in Depression, Anxiety, and Stress	suicide, as will be described later. In contrast, multiple animal studies have shown that the…
19	8. Cannabinoids in Depression and Anxiety — 8.2. Evidence for the Involvement of the ECS in Depression, Anxiety, and Stress	Models of depression and anxiety involving stress have shown that the function of the ECS is…

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In this knowledge base

Title	Year	PMID
A Prospective Comparison of Bipolar I and II Subjects with and without Comorbid Cannabis Use Disorders from the COGA Dataset.	2023	37626487

External

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Frequency of cannabis use and symptoms of anxiety and depression: a cross-sectional analysis of the Colorado cannabis users health cohort.	Steeger CM et al.	—	2025	→
Future Directions in Anxiolytic Therapy: A Comprehensive Review of Novel Targets and Strategies.	Mahima et al.	—	2025	→
Gastrodin Ameliorates Post-Stroke Depressive-Like Behaviors Through Cannabinoid-1 Receptor-Dependent PKA/RhoA Signaling Pathway.	Wang S et al.	—	2025	→
Genetic characterization of the endocannabinoid system and psychiatric features in patients with migraine and medication overuse headache.	Romozzi M et al.	—	2025	→
Inhibition of an endocannabinoid catabolizing enzyme is a potential mechanism for the anxiolytic effect of chamomile.	El-Alfy AT et al.	—	2025	→
Medicinal cannabis in the management of anxiety disorders: A systematic review.	Roberts L et al.	—	2025	→
Phytocannabinoids restore seizure-induced alterations in emotional behaviour in male rats.	Gom RC et al.	—	2025	→
Serum Lipidome Change in Japanese Patients with Major Depressive Disorder: A Real-World Exploratory Study.	Okamoto N et al.	—	2025	→
Association between cannabis use and physical activity in the United States based on legalization and health status.	Merrill RM et al.	—	2024	→
CBD-Loaded Nanostructured Lipid Carriers: Optimization, Characterization, and Stability.	Xie Y et al.	—	2024	→
Endocannabinoid System and Metabolism: The Influences of Sex.	Forner-Piquer I et al.	—	2024	→
Genome-wide meta-analyses of non-response to antidepressants identify novel loci and potential drugs	Koch E et al.	—	2024	—
Immunomodulatory effects of cannabinoids against viral infections: a review of its potential use in SARS-CoV2 infection.	Hassan Kalantar Neyestanaki M et al.	—	2024	→
Interactions between metabotropic glutamate and CB1 receptors: implications for mood, cognition, and synaptic signaling based on data from mGluR and CB1R-targeting drugs.	Stachowicz K	—	2024	→
New insights into the involvement of serotonin and BDNF-TrkB signalling in cannabidiol's antidepressant effect.	Guldager MB et al.	—	2024	→
Peripheral endocannabinoids in major depressive disorder and alcohol use disorder: a systematic review.	Fuentes JJ et al.	—	2024	→
Pharmacovigilance of unlicensed cannabidiol in European countries.	Calapai F et al.	—	2024	→
Role of T and B lymphocyte cannabinoid type 1 and 2 receptors in major depression and suicidal behaviours.	Maes M et al.	—	2024	→
The Interplay of Exogenous Cannabinoid Use on Anandamide and 2-Arachidonoylglycerol in Anxiety: Results from a Quasi-Experimental Ad Libitum Study.	Martin-Willett R et al.	—	2024	→
Therapeutic potential of cannabidiol in depression.	Guldager MB et al.	—	2024	→
Therapeutic use of medical Cannabis in neurological diseases: a clinical update.	Hidding U et al.	—	2024	→
The Use of Compounds Derived from <i>Cannabis sativa</i> in the Treatment of Epilepsy, Painful Conditions, and Neuropsychiatric and Neurodegenerative Disorders.	Stasiłowicz-Krzemień A et al.	—	2024	→
UK Medical Cannabis Registry: a cohort study of patients prescribed cannabis-based oils and dried flower for generalised anxiety disorder.	Warner-Levy J et al.	—	2024	→
A Prospective Comparison of Bipolar I and II Subjects with and without Comorbid Cannabis Use Disorders from the COGA Dataset.	Preuss UW et al.	—	2023	→
Challenges and considerations for treating PTSD with medicinal cannabis: the Australian clinician's perspective.	Ney LJ et al.	—	2023	→
Deciphering the mechanisms of reciprocal regulation or interdependence at the cannabinoid CB1 receptors and cyclooxygenase-2 level: Effects on mood, cognitive implications, and synaptic signaling.	Stachowicz K	—	2023	→
Psychological Interventions for Cannabis Use among Adolescents and Young Adults: A Systematic Review.	Bou Nassif Y et al.	—	2023	→