6-Benzhydryl-4-amino-quinolin-2-ones as Potent Cannabinoid Type 1 (CB<sub>1</sub>) Receptor Inverse Agonists and Chemical Modifications for Peripheral Selectivity

Yue-mei, Zhang; Greco, Michael N.; Macielag, Mark J.; Teleha, Christopher A.; DesJarlais, Renée L.; Tang, Yuting; Ho, George; Hou, Cuifen; Chen, Cailin; Zhao, Shuyuan; Kauffman, Jack A.; Camacho, Raul C.; Qi, Jenson; Murray, William V.; Demarest, Keith T.; Leonard, Janet L.

doi:10.1021/acs.jmedchem.8b01467

Cited by 13 publications

(10 citation statements)

References 46 publications

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“…With a considerably lower exposure in the brain, Compound D4, developed by 7TM Pharma, induced pronounced weight reduction in a dose-dependent manner in obese mice in comparison with rimonabant [146]. Although designed to be a P-glycoprotein (P-gp) substrate in order to decrease its brain penetration, Compound 6a, developed by Janssen Research & Development, accumulated in the brain following chronic administration, suggesting that its in vivo metabolic efficacy cannot exclude blocking central CB 1 Rs [147]. Compound 2p, which originated from the brain-penetrant CB 1 R inverse agonist program of the same group, reduced glucose levels without centrally mediated behavioral effects and a reduction in food intake or body weight [148].…”

Section: Current View Regarding Novel Peripherally Restricted Cb1rmentioning

confidence: 99%

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Hirsch

Tam

2019

Toxins

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In this review, we discuss the role of the endocannabinoid (eCB) system in regulating energy and metabolic homeostasis. Endocannabinoids, via activating the cannabinoid type-1 receptor (CB1R), are commonly known as mediators of the thrifty phenotype hypothesis due to their activity in the central nervous system, which in turn regulates food intake and underlies the development of metabolic syndrome. Indeed, these findings led to the clinical testing of globally acting CB1R blockers for obesity and various metabolic complications. However, their therapeutic potential was halted due to centrally mediated adverse effects. Recent observations that highlighted the key role of the peripheral eCB system in metabolic regulation led to the preclinical development of various novel compounds that block CB1R only in peripheral organs with very limited brain penetration and without causing behavioral side effects. These unique molecules, which effectively ameliorate obesity, type II diabetes, fatty liver, insulin resistance, and chronic kidney disease in several animal models, are likely to be further developed in the clinic and may revive the therapeutic potential of blocking CB1R once again.

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Section: Current View Regarding Novel Peripherally Restricted Cb1rmentioning

confidence: 99%

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Hirsch

Tam

2019

Toxins

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“…An important factor supporting THCV use in therapy could also be its antipsychotic effect [180]. Other compounds with same pharmacodynamics, i.e., able to influence feeding behaviour, which still require further research include: NESS06SM [181], SM-11 [182], PIMSR [183], BAR-1 [184], Compound10q [185], Compound2c [186], Com-pound5 [172], Compound13 [165], Compound6a [187], and CompoundD4 [188]. These were designed to have low penetration in the brain, except for Compound6a, whose chronic administration caused accumulation in the brain [187].…”

Section: Endocannabinoid System As a Pharmacological Target For Obesity And Food Addictionmentioning

confidence: 99%

“…Other compounds with same pharmacodynamics, i.e., able to influence feeding behaviour, which still require further research include: NESS06SM [181], SM-11 [182], PIMSR [183], BAR-1 [184], Compound10q [185], Compound2c [186], Com-pound5 [172], Compound13 [165], Compound6a [187], and CompoundD4 [188]. These were designed to have low penetration in the brain, except for Compound6a, whose chronic administration caused accumulation in the brain [187]. On the other hand, clinical studies demonstrated decreased body weight and a safe administration profile for two other CB1 antagonists: AVE-1625 [174] and SLV-319 [189].…”

Section: Endocannabinoid System As a Pharmacological Target For Obesity And Food Addictionmentioning

confidence: 99%

Obesity as a Condition Determined by Food Addiction: Should Brain Endocannabinoid System Alterations Be the Cause and Its Modulation the Solution?

et al. 2021

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Obesity is a complex disorder, and the number of people affected is growing every day. In recent years, research has confirmed the hypothesis that food addiction is a determining factor in obesity. Food addiction is a behavioral disorder characterized by disruptions in the reward system in response to hedonic eating. The endocannabinoid system (ECS) plays an important role in the central and peripheral control of food intake and reward-related behaviors. Moreover, both obesity and food addiction have been linked to impairments in the ECS function in various brain regions integrating peripheral metabolic signals and modulating appetite. For these reasons, targeting the ECS could be a valid pharmacological therapy for these pathologies. However, targeting the cannabinoid receptors with inverse agonists failed when used in clinical contexts as a consequence of the induction of affective disorders. In this context, new classes of drugs acting either on CB1 and/or CB2 receptors or on synthetic and degradation enzymes of endogenous cannabinoids are being studied. However, further investigation is necessary to find safe and effective treatments that can exert anti-obesity effects, normalizing reward-related behaviors without causing important adverse mood effects.

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“…MRI-1867 is a low brain penetrating CB1 inverse agonist developed for the treatment of liver fibrosis, and DIO mice treated with MRI-1867 for 28 days experienced significant reductions in body weight and food intake, and increased energy expenditure [ 68 , 170 ]. Other similar compounds include Compound 6a, BMS-725519, BMS-811064, and BMS-812204 [ 73 , 171 ]. All of these novel compounds require further investigation.…”

Section: Exploring the Direct Effects Of Cannabinoid Drugs On Bodymentioning

confidence: 99%

Targeting the Endocannabinoid CB1 Receptor to Treat Body Weight Disorders: A Preclinical and Clinical Review of the Therapeutic Potential of Past and Present CB1 Drugs

Murphy

Foll

2020

Biomolecules

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Obesity rates are increasing worldwide and there is a need for novel therapeutic treatment options. The endocannabinoid system has been linked to homeostatic processes, including metabolism, food intake, and the regulation of body weight. Rimonabant, an inverse agonist for the cannabinoid CB1 receptor, was effective at producing weight loss in obese subjects. However, due to adverse psychiatric side effects, rimonabant was removed from the market. More recently, we reported an inverse relationship between cannabis use and BMI, which has now been duplicated by several groups. As those results may appear contradictory, we review here preclinical and clinical studies that have studied the impact on body weight of various cannabinoid CB1 drugs. Notably, we will review the impact of CB1 inverse agonists, agonists, partial agonists, and neutral antagonists. Those findings clearly point out the cannabinoid CB1 as a potential effective target for the treatment of obesity. Recent preclinical studies suggest that ligands targeting the CB1 may retain the therapeutic potential of rimonabant without the negative side effect profile. Such approaches should be tested in clinical trials for validation.

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6-Benzhydryl-4-amino-quinolin-2-ones as Potent Cannabinoid Type 1 (CB₁) Receptor Inverse Agonists and Chemical Modifications for Peripheral Selectivity

Cited by 13 publications

References 46 publications

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Obesity as a Condition Determined by Food Addiction: Should Brain Endocannabinoid System Alterations Be the Cause and Its Modulation the Solution?

Targeting the Endocannabinoid CB1 Receptor to Treat Body Weight Disorders: A Preclinical and Clinical Review of the Therapeutic Potential of Past and Present CB1 Drugs

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6-Benzhydryl-4-amino-quinolin-2-ones as Potent Cannabinoid Type 1 (CB1) Receptor Inverse Agonists and Chemical Modifications for Peripheral Selectivity

Cited by 13 publications

References 46 publications

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Cannabis: From a Plant That Modulates Feeding Behaviors toward Developing Selective Inhibitors of the Peripheral Endocannabinoid System for the Treatment of Obesity and Metabolic Syndrome

Obesity as a Condition Determined by Food Addiction: Should Brain Endocannabinoid System Alterations Be the Cause and Its Modulation the Solution?

Targeting the Endocannabinoid CB1 Receptor to Treat Body Weight Disorders: A Preclinical and Clinical Review of the Therapeutic Potential of Past and Present CB1 Drugs

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Product

Resources

About

6-Benzhydryl-4-amino-quinolin-2-ones as Potent Cannabinoid Type 1 (CB₁) Receptor Inverse Agonists and Chemical Modifications for Peripheral Selectivity