Your search keyword '"Soubrié P"' showing total 3 results

1. SGIP1 is involved in regulation of emotionality, mood, and nociception and modulates in vivo signalling of cannabinoid CB1 receptors.

Author

Dvorakova, Michaela, Kubik‐Zahorodna, Agnieszka, Straiker, Alex, Sedlacek, Radislav, Hajkova, Alena, Mackie, Ken, Blahos, Jaroslav, and Kubik-Zahorodna, Agnieszka

Subjects

CYCLOSERINE, CANNABINOID receptors, ENDORPHIN receptors, PROCESS control systems, SHORT-term memory, ANXIETY, NERVOUS system, RESEARCH, ANIMAL experimentation, RESEARCH methodology, SENSORY perception, CELL receptors, FEAR, MEDICAL cooperation, EVALUATION research, HYDROCARBONS, COMPARATIVE studies, MICE

Abstract

Background and Purpose: Src homology 3-domain growth factor receptor-bound 2-like endophilin interacting protein 1 (SGIP1) interacts with cannabinoid CB1 receptors. SGIP1 is abundantly and principally expressed within the nervous system. SGIP1 and CB1 receptors co-localize in axons and presynaptic boutons. SGIP1 interferes with the internalization of activated CB1 receptors in transfected heterologous cells. Consequently, the transient association of CB1 receptors with β-arrestin2 is enhanced and prolonged, and CB1 receptor-mediated ERK1/2 signalling is decreased. Because of these actions, SGIP1 may modulate affect, anxiety, pain processing, and other physiological processes controlled by the endocannabinoid system (ECS).Experimental Approach: Using a battery of behavioural tests, we investigated the consequences of SGIP1 deletion in tasks regulated by the ECS in SGIP1 constitutive knockout (SGIP1-/- ) mice.Key Results: In SGIP1-/- mice, sensorimotor gating, exploratory levels, and working memory are unaltered. SGIP1-/- mice have decreased anxiety-like behaviours. Fear extinction to tone is facilitated in SGIP1-/- females. Several cannabinoid tetrad behaviours are altered in the absence of SGIP1. SGIP1-/- males exhibit abnormal behaviours on Δ9 -tetrahydrocannabinol withdrawal. SGIP1 deletion also reduces acute nociception, and SGIP1-/- mice are more sensitive to analgesics.Conclusion and Implications: SGIP1 was detected as a novel protein associated with CB1 receptors, and profoundly modified CB1 receptor signalling. Genetic deletion of SGIP1 particularly affected behavioural tests of mood-related assessment and the cannabinoid tetrad. SGIP1-/- mice exhibit decreased nociception and augmented responses to CB1 receptor agonists and morphine. These in vivo findings suggest that SGIP1 is a novel modulator of CB1 receptor-mediated behaviour. [ABSTRACT FROM AUTHOR]

Published

2021

2. β-Caryophyllene, a dietary terpenoid, inhibits nicotine taking and nicotine seeking in rodents.

Author

He, Yi, Galaj, Ewa, Bi, Guo‐Hua, Wang, Xiao‐Fei, Gardner, Eliot, Xi, Zheng‐Xiong, Bi, Guo-Hua, Wang, Xiao-Fei, and Xi, Zheng-Xiong

Subjects

DOPAMINERGIC neurons, NICOTINE, CARYOPHYLLENE, SMOKING cessation, ANIMAL behavior, RODENTS, CANNABINOID receptors, FOOD additives, TERPENES, ANIMAL experimentation, CELL receptors, RATS, RESEARCH funding, MICE

Abstract

Background and Purpose: β-Caryophyllene (BCP) is a plant-derived terpenoid used as a food additive for many decades. Recent studies indicate that BCP is a cannabinoid CB2 receptor agonist with medical benefits for a number of human diseases. However, little is known about its therapeutic potential for drug abuse and addiction.Experiment Approach: We used pharmacological, transgenic, and optogenetic approaches to systematically evaluate the effects of BCP on nicotine-taking and nicotine-seeking behaviour in animal models of drug self-administration, electrical, and optical brain-stimulation reward.Key Results: Systemic administration of BCP dose-dependently inhibited nicotine self-administration and motivation for nicotine seeking in rats and mice. The reduction in nicotine self-administration was blocked by AM630, a selective CB2 receptor antagonist, but not by AM251, a selective CB1 receptor antagonist, suggesting involvement of a CB2 receptor mechanism. Genetic deletion of CB2 receptors in mice blocked the reduction in nicotine self-administration produced only by low doses, but not by high doses, of BCP, suggesting involvement of both CB2 and non-CB2 receptor mechanisms. Furthermore, in the intracranial self-stimulation paradigm, BCP attenuated electrical brain-stimulation reward and nicotine-enhanced brain-stimulation reward in rats. Lastly, BCP also attenuated brain-stimulation reward maintained by optogenetic stimulation of dopaminergic neurons in the ventral tegmental area in DAT-cre mice, suggesting the involvement of a dopamine-dependent mechanism in BCP's action.Conclusions and Implications: The present findings suggest that BCP has significant anti-nicotine effects via both CB2 and non-CB2 receptor mechanisms and, therefore, deserves further study as a potential new pharmacotherapy for cigarette smoking cessation. [ABSTRACT FROM AUTHOR]

Published

2020

3. Dual inhibition of cannabinoid CB1 receptor and inducible NOS attenuates obesity-induced chronic kidney disease.

Author

Udi, Shiran, Hinden, Liad, Ahmad, Majdoleen, Drori, Adi, Iyer, Malliga R., Cinar, Resat, Herman‐Edelstein, Michal, Tam, Joseph, and Herman-Edelstein, Michal

Subjects

CHRONIC kidney failure, KIDNEY tubules, CANNABINOID receptors, WESTERN diet, OXIDATIVE stress, PREVENTION of obesity, OBESITY, RESEARCH, ANIMAL experimentation, RESEARCH methodology, CELL receptors, DIET, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, CELLS, RESEARCH funding, OXIDOREDUCTASES, MICE, CHEMICAL inhibitors

Abstract

Background and Purpose: Obesity, an important risk factor for developing chronic kidney disease (CKD), affects the kidneys by two main molecular signalling pathways: the endocannabinoid/CB1 receptor system, whose activation in obesity promotes renal inflammation, fibrosis, and injury, and the inducible NOS (iNOS), which generates ROS resulting in oxidative stress. Hence, a compound that inhibits both peripheral CB1 receptors and iNOS may serve as an effective therapeutic agent against obesity-induced CKD.Experimental Approach: Here, we describe the effect of a novel peripherally restricted, orally bioavailable dual CB1 receptor/iNOS antagonist, MRI-1867 (3 mg·kg-1 ), in ameliorating obesity-induced CKD, and compared its metabolic and renal efficacies to a stand-alone peripheral CB1 receptor antagonist (JD5037; 3 mg·kg-1 ), iNOS antagonist (1400W; 10 mg·kg-1 ), and pair feeding. Mice with high-fat diet-induced obesity were treated orally with these compounds or vehicle (Veh) for 28 days. Standard diet-fed mice treated with Veh served as controls.Key Results: Enhanced expression of CB1 receptors and iNOS in renal tubules was found in human kidney patients with obesity and other CKDs. The hybrid inhibitor ameliorated obesity-induced kidney morphological and functional changes via decreasing kidney inflammation, fibrosis, oxidative stress, and renal injury. Some of these features were independent of the improved metabolic profile mediated via inhibition of CB1 receptors. An additional interesting finding is that these beneficial effects on the kidney were partially associated with modulating renal adiponectin signalling.Conclusions and Implications: Collectively, our results highlight the therapeutic relevance of blocking CB1 receptors and iNOS in ameliorating obesity-induced CKD. [ABSTRACT FROM AUTHOR]

Published

2020