Endocannabinoids: Stress, Anxiety, and Fear

A recent meta-analysis of studies related to ligand binding affinity and receptor distribution for the CB ₁ receptor indicates important differences between species and among analytic techniques. 24 In vitro binding studies for the CB ₁ receptor found differences in binding potential from many factors including tissue state (e.g., brain sections versus brain homogenates), tissue type (e.g., native versus transfected cells), and species. Receptor distribution also varied by method, with in situ hybridization differing considerably from autoradiographic and immunocytochemical studies, which were in rough agreement. Of particular importance, ordering brain structures by receptor density resulted in different rank ordering in human and rat. 24 Maps of the approximate regional cannabinoid receptor density in primate (human and nonhuman) brain is illustrated in the cover art and Figure 1 . 1 – 4 The relative sensitivities of GABA-ergic and glutaminergic neurons may also vary by species. 15 Endogenous ligands (endocannabinoids) for the CB ₁ receptor act presynaptically to inhibit release of a wide range of neurotransmitters including glutamate, acetylcholine, norepinephrine, and GABA ( Figure 2 ). 7, 15, 25 These compounds are not synthesized in advance and stored. Rather, they are synthesized in the postsynaptic cell in response to depolarization. This is thus an “on-demand” system, with synthesis occurring only when and where it is required. 10 Endocannabinoids are released by an unknown mechanism and diffuse across the synapse to activate receptors located on the axon terminal, suppressing neuronal excitability and inhibiting neurotransmission. They are inactivated rapidly by uptake (possibly carrier mediated) followed by intracellular hydrolysis [fatty acid amide hydrolase (FAAH), monoacylglycerol lipase (MGL)]. 6, 7, 10, 15, 18, 26 The two most studied endocannabinoids are anandamide and 2-arachidonoylglycerol (2-AG). Both anandamide and Δ9 THC are low intrinsic activity (partial) agonists for the CB1 receptor. 2-AG is a high intrinsic activity (full) agonist. 16 Of particular importance, synthetic compounds delivered systemically may not have the same effects as endogenous compounds, as they lack both spatial and temporal specificity. 10, 27 This may be one reason why some studies have found a bell-shaped or biphasic relationship between dose and effect, with high doses often having the opposite effect of low doses. 10, 14, 27, 28

The potential interactions between ligands and receptors are complex. 15, 16 Most receptors have both active and inactive conformations. If a particular ligand favors the active conformation of the receptor it is considered to have high intrinsic activity (full agonist). If a ligand does not favor the active conformation then at the same level of receptor occupancy there will be a lower level of activation because some receptors will be in the active state while others will be in the inactive state. Such a ligand is considered to have low intrinsic activity (partial agonist). A third type of interaction is possible in the endocannabinoid system, because at least some portions of it are tonically active. Thus a ligand can actually decrease activity below normal levels (inverse agonist). In addition, particular ligands are able to activate one signaling pathway more than another. This is referred to as agonist-directed trafficking or functional selectivity. Thus, different agonists may favor coupling to different G proteins.

The endocannabinoids are neuromodulatory compounds that provide feedback inhibition via CB ₁ receptors and are integral to many types of synaptic plasticity. 10, 17, 18 The first to be identified were depolarization-induced suppression of inhibition (DSI) in the hippocampus and depolarization-induced suppression of excitation (DSE) in the cerebellum. 17 Endocannabinoid synthesis is stimulated by the increased intracellular calcium that occurs as a result of depolarization of the postsynaptic dendrite for both DSI and DSE, which occur widely in the brain. 18 Activation of metabotropic glutamate or muscarinic receptors can also stimulate endocannabinoid synthesis at both excitatory and inhibitory synapses. These have been termed metabotropic suppression of inhibition (MSI) and metabotropic suppression of excitation (MSE). 18 Although not dependent on a postsynaptic increase in calcium, both MSE and MSI are enhanced by increased calcium and thus may serve as coincidence detectors. An alternative name for this type of plasticity is endocannabinoid-mediated short-term depression (eCB-STD). 17 Endocannabinoids also mediate some types of long-term depression (LTD) in multiple areas, including hippocampus, dorsal striatum, ventral striatum (nucleus accumbens), cerebellum, and prefrontal cortex. 17, 18, 29 Endocannabinoids can also act on somatic receptors, activating potassium channels, thus depolarizing the neuron and inhibiting action potential generation. 17, 18

The endocannabinoid system participates in multiple brain circuits implicated in neuropsychiatric conditions such as those modulating stress reactions, learning, and extinction of fear, emotional regulation, and reward processes. 31, 32 CB ₁ receptors are found in many areas involved in regulation of the stress response including the paraventricular nucleus (PVN) of the hypothalamus, corticotroph cells in the pituitary, adrenal glands, and limbic-related areas of the brain. 30 Endocannabinoids inhibit the hypothalamic-pituitary-adrenal (HPA) axis and may well provide an ongoing basal level of inhibition. During acute stress, corticotrophin releasing factor is released into the portal system by neurons in the paraventricular nucleus. Corticotrophin releasing factor (CRF) induces release of adrenocorticotrophic hormone from the anterior pituitary. Adrenocorticotrophic hormone stimulates production of glucocorticoids (e.g., corticosterone) in the adrenal gland. Glucocorticoids, in turn, inhibit release of corticotrophin releasing factor in the hypothalamus and adrenocorticotrophic hormone (ACTH) in the pituitary. Negative feedback in the hypothalamus is mediated by glucocorticoid-stimulated synthesis and release of endocannabinoids within the paraventricular nucleus. 10, 25, 30 Thus, endocannabinoids are released in response to activity in the hypothalamic-pituitary-adrenal axis and serve to bring it back toward its baseline (prestress) state. 10

Animal studies indicate that neither acute stress nor chronic predictable stress (which will habituate) alter CB ₁ receptor density or affinity in the brain. 33 Both chronic unpredictable stress (which does not habituate) and chronic administration of corticosterone, on the other hand, decrease CB ₁ receptor density in the hippocampus. 33 These stress conditions also differentially alter the content of 2-AG and anandamide of many brain regions. Some studies support the theory that a progressive increase of 2-AG and decrease of anandamide within limbic-related brain areas (e.g., medial prefrontal cortex, limbic forebrain, amygdala, hypothalamus) may, in part, mediate behavioral habituation to chronic predictable stress. 33 An opposite pattern (increased anandamide, decreased 2-AG) is seen in the ventral striatum, which may have implications for endocannabinoid-mediated facilitation of reward. 33 An antidepressant-like effect (as indicated by enhanced stress-coping behaviors and decreased anhedonic behaviors), has been reported for both compounds that directly activate CB ₁ receptors and those that prolong the action of naturally released endocannabinoids (e.g., inhibit uptake, inhibit hydrolysis). 28 Animal studies of social defeat stress (which produces symptoms of anxiety and depression) indicate that it decreases CB ₁ receptor-mediated inhibition of GABA (but not glutamate) neurotransmission in the striatum. 34 This change occurs as a result of stress-induced increases in glucocorticoids, and can be reversed by both natural rewards (e.g., access to sucrose) and administration of drugs with rewarding properties (e.g., cocaine). 34 An important role for the endocannabinoid system in reward-related processes is likely. CB ₁ receptor-activation modulates dopamine signaling in both the ventral tegmental area and the ventral striatum. 13, 29 CB ₁ receptors also participate in LTD at glutaminergic synapses in both dorsal and ventral striatum. 29 It has been proposed that the endocannabinoid system provides the common neurobiological mechanism underlying both the rewarding aspects of drugs of abuse and relapse, suggesting that blockade of CB ₁ receptors may have therapeutic potential. 13, 35 Studies also support the involvement of the endocannabinoid system in extinction of conditioned fear. 10, 25, 28 Endocannabinoid content of the amygdala is increased following exposure to the conditioned stimulus (e.g., tone previously paired to foot shock). 25, 28 Removal of the influence of CB ₁ receptors (either by pharmacological blockade or by genetic manipulation) impairs extinction of conditioned fear. 27, 28 Extinction is enhanced by administration of compounds that directly activate CB ₁ receptors or prolong the action of naturally released endocannabinoids (e.g., inhibit uptake, inhibit hydrolysis). 10, 27, 28

There is growing evidence that another important function of the endocannabinoid system is regulation of energy balance, both in terms of influencing appetite and by modulating metabolism. 36 – 39 Both central and peripheral actions are likely to be involved. CB ₁ receptors are present in hypothalamic areas (e.g., mediobasal, paraventricular, lateral) integral to balancing energy intake with energy expenditure. 38 Endocannabinoid levels in the hypothalamus are increased by starvation and decreased by food intake. 36 In rats, food intake is increased following administration of endocannabinoids to either the hypothalamus or mesolimbic forebrain. 36 In addition, studies in both humans and animals have found that that blockade of CB ₁ receptors normalizes several metabolic parameters that are risk factors for metabolic syndrome (e.g., decreased triglycerides and insulin resistance, increased high-density lipoprotein cholesterol) in excess of what would be expected from weight loss alone, supporting a role in glucose homeostasis and adipose tissue metabolism. 36 – 40 Research suggests that this system may be overactive in conditions such as obesity and hyperglycemia. 36, 38, 39, 41 CB ₁ receptor activation increases fatty acid synthesis in the liver as well as lipid synthesis by adipose tissue, and obesity is associated with increases in CB ₁ receptors in both adipose tissue and skeletal muscle. 36

The involvement of the endocannabinoid system in multiple aspects of brain function provides new targets for the development of novel therapeutic agents for a wide range of psychiatric disorders. 9, 14 Potential applications include treatment of mood and anxiety disorders, degenerative conditions, and acquired brain injuries. 9, 10, 14, 19, 23, 25, 42 – 46 In addition to receptor ligands (both agonists and antagonists), a number of compounds have been developed that prolong endocannabinoid action, either by inhibiting uptake or by decreasing hydrolysis. 6, 9, 15, 26 One challenge is to develop agents that are both selective and safe. The difficulty in achieving this has recently been driven home by the European Medicines Agency’s decision to suspend sales of rimonabant (CB ₁ receptor antagonist/inverse agonist), approved 2 years ago for the treatment of obesity, citing adverse psychiatric effects. 47

Presented at the American Neuropsychiatric Association Annual Meeting, San Antonio, Texas, February 19–22, 2009.