Lack of presynaptic interaction between glucocorticoid and CB1 cannabinoid receptors in GABA- and glutamatergic terminals in the frontal cortex of laboratory rodents

Bitencourt, Rafael Mariano de; Alpár, Alán; Cinquina, Valentina; Ferreira, Samira G.; Pinheiro, Bárbara S.; Lemos, Cristina; Ledent, Catherine; Takahashi, Reinaldo Ν.; Sialana, Fernando J.; Lubec, Gert; Cunha, Rodrigo A.; Harkany, Tibor; Köfalvi, Attila

doi:10.1016/j.neuint.2015.07.014

Cited by 10 publications

(5 citation statements)

References 81 publications

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“…Notwithstanding, a recent characterization of O-2050 revealed some unexpected in vitro partial agonist activity in cyclic AMP assay, and a lack of antagonism on in vivo effects of Δ 9 -THC and WIN55212-2 [393]. In our hands, O-2050 (1 µM) had no effect on the depolarizationinduced release of GABA, glutamate and serotonin in the frontal cortex [396,397], and prevented the inhibitory action of WIN55212-2. In that sense, it mimicked the effect of the genetic deletion of the CB 1 R and we concluded that O-2050 is a useful in vitro CB 1 R antagonist up to the concentration of 1 µM.…”

Section: Multifaceted Interaction Of Ligands and G Proteins With The contrasting

confidence: 47%

“…Steroid hormones interact with the endocannabinoid system, which has significant therapeutic potential. One important feature of glucocorticoid receptors (GcRs) is that they co-localize with DAGLα in post-synaptic neural compartments apposing CB 1 R-positive nerve terminals in the brain [397]. GcR activation in the prefrontal cortex triggers endocannabinoid release [966], which in turn downregulates the hypothalamo-pituitary-adrenal (HPA) axis to decrease circulating corticosteroid levels [967,968], facilitate the extinction and impair the retrieval of aversive memories [965,967,[969][970][971].…”

Section: δ 9 -Thc and Steroid Hormonesmentioning

confidence: 99%

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Cannabis: A Treasure Trove or Pandora's Box?

Solymosi

Köfalvi

2017

MRMC

122

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We summarize our current knowledge on the recreational use of cannabis with respect to the modes of consumption, short-term effects, chronic health consequences and cannabis use disorder. Next, we overview the molecular targets of a dozen major and minor bioactive cannabinoids in the body. This helps us introduce the endocannabinoid system in an unprecedented detail: its up-todate molecular biology, pharmacology, physiology and medical significance, and beyond. In conclusion, we offer an unbiased survey about cannabis to help better weigh its medical value versus the associated risks.

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Section: Multifaceted Interaction Of Ligands and G Proteins With The contrasting

confidence: 47%

Section: δ 9 -Thc and Steroid Hormonesmentioning

confidence: 99%

Cannabis: A Treasure Trove or Pandora's Box?

Solymosi

Köfalvi

2017

MRMC

122

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“…2). Like in the hypothalamus, recent data indicate that the GR in the frontal cortex are expressed on postsynaptic profiles (3). Excitatory projections from these brain regions accelerate the poststress decline in circulating glucocorticoids likely through activation of inhibitory inputs from the bed nucleus of the stria terminalis to the PVN (31, 35).…”

Section: Glucocorticoids Affect Synaptic Plasticity Via Endogenous Cbmentioning

confidence: 99%

Endocannabinoid Signaling and the Hypothalamic‐Pituitary‐Adrenal Axis

Hillard

Beatka

Sarvaideo

2016

Comprehensive Physiology

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The elucidation of Δ9-tetrahydrocannabinol as the active principal of Cannabis sativa in 1963 initiated a fruitful half-century of scientific discovery, culminating in the identification of the endocannabinoid signaling system, a previously unknown neuromodulatory system. A primary function of the endocannabinoid signaling system is to maintain or recover homeostasis following psychological and physiological threats. We provide a brief introduction to the endocannabinoid signaling system and its role in synaptic plasticity. The majority of the article is devoted to a summary of current knowledge regarding the role of endocannabinoid signaling as both a regulator of endocrine responses to stress and as an effector of glucocorticoid and corticotrophin-releasing hormone signaling in the brain. We summarize data demonstrating that cannabinoid receptor 1 (CB1R) signaling can both inhibit and potentiate the activation of the hypothalamic-pituitary-adrenal axis by stress. We present a hypothesis that the inhibitory arm has high endocannabinoid tone and also serves to enhance recovery to baseline following stress, while the potentiating arm is not tonically active but can be activated by exogenous agonists. We discuss recent findings that corticotropin-releasing hormone in the amygdala enables hypothalamic-pituitary-adrenal axis activation via an increase in the catabolism of the endocannabinoid N-arachidonylethanolamine. We review data supporting the hypotheses that CB1R activation is required for many glucocorticoid effects, particularly feedback inhibition of hypothalamic-pituitary-adrenal axis activation, and that glucocorticoids mobilize the endocannabinoid 2-arachidonoylglycerol. These features of endocannabinoid signaling make it a tantalizing therapeutic target for treatment of stress-related disorders but to date, this promise is largely unrealized.

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“…Neuromodulators enhance the flexibility of neural networks by multiple mechanisms. These include the regulation of intrinsic properties (i.e., pre-existing conductances; Benson and Levitan, 1983 ; Kiehn and Harris-Warrick, 1992a , b ; Harris-Warrick et al, 1995 ; Galbavy et al, 2013 ), modulating synaptic properties ( Johnson et al, 1993a , b,1995 ; Zhao et al, 2011 ; Bitencourt et al, 2015 ; Böhm et al, 2015 ), reconfiguring participating neurons within the network ( Hooper and Moulins, 1989 ; Fénelon et al, 1998 ; Lieske et al, 2000 ), and modulating plasticity and even modulation itself ( Mesce, 2002 ; McLean and Sillar, 2004 ; Zhou et al, 2007 ; Pawlak et al, 2010 ; Lawrence et al, 2015 ). Another important mechanism of the regulation of neuronal excitability is the modulation of leak currents ( Bayliss et al, 1992 ; Erxleben et al, 1995 ; Talley et al, 2000 ; Cymbalyuk et al, 2002 ; Xu et al, 2009 ), and of the ratio of leak current to pacemaking current amplitude (and not just the pacemaking current amplitude), as is the case in the regulation of pacemaking activity in the pre-Bötzinger complex ( Del Negro et al, 2002 ).…”

Section: Introductionmentioning

confidence: 99%

Voltage Dependence of a Neuromodulator-Activated Ionic Current

Gray

Golowasch

2016

eneuro

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The neuromodulatory inward current (IMI) generated by crab Cancer borealis stomatogastric ganglion neurons is an inward current whose voltage dependence has been shown to be crucial in the activation of oscillatory activity of the pyloric network of this system. It has been previously shown that IMI loses its voltage dependence in conditions of low extracellular calcium, but that this effect appears to be regulated by intracellular calmodulin. Voltage dependence is only rarely regulated by intracellular signaling mechanisms. Here we address the hypothesis that the voltage dependence of IMI is mediated by intracellular signaling pathways activated by extracellular calcium. We demonstrate that calmodulin inhibitors and a ryanodine antagonist can reduce IMI voltage dependence in normal Ca2+, but that, in conditions of low Ca2+, calmodulin activators do not restore IMI voltage dependence. Further, we show evidence that CaMKII alters IMI voltage dependence. These results suggest that calmodulin is necessary but not sufficient for IMI voltage dependence. We therefore hypothesize that the Ca2+/calmodulin requirement for IMI voltage dependence is due to an active sensing of extracellular calcium by a GPCR family calcium-sensing receptor (CaSR) and that the reduction in IMI voltage dependence by a calmodulin inhibitor is due to CaSR endocytosis. Supporting this, preincubation with an endocytosis inhibitor prevented W7 (N-(6-aminohexyl)-5-chloro-1-naphthalenesulfonamide hydrochloride)-induced loss of IMI voltage dependence, and a CaSR antagonist reduced IMI voltage dependence. Additionally, myosin light chain kinase, which is known to act downstream of the CaSR, seems to play a role in regulating IMI voltage dependence. Finally, a Gβγ-subunit inhibitor also affects IMI voltage dependence, in support of the hypothesis that this process is regulated by a G-protein-coupled CaSR.

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Lack of presynaptic interaction between glucocorticoid and CB1 cannabinoid receptors in GABA- and glutamatergic terminals in the frontal cortex of laboratory rodents

Cited by 10 publications

References 81 publications

Cannabis: A Treasure Trove or Pandora's Box?

Cannabis: A Treasure Trove or Pandora's Box?

Endocannabinoid Signaling and the Hypothalamic‐Pituitary‐Adrenal Axis

Voltage Dependence of a Neuromodulator-Activated Ionic Current

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