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3. Erratum: Synthesis and quantitative structure-activity relationship of fatty acid amide hydrolase inhibitors: Modulation at the N-portion of biphenyl-3-yl alkylcarbamates (Journal of Medicinal Chemistry (2008) 51 (3487))

Author

Mor, M, Lodola, A, Rivara, S, Vacondio, F, Duranti, A, Tontini, A, Sanchini, S, Piersanti, G, Clapper, JR, King, AR, Tarzia, G, and Piomelli, D

Subjects
Medicinal & Biomolecular Chemistry, Medicinal and Biomolecular Chemistry, Pharmacology and Pharmaceutical Sciences, Organic Chemistry
Published
2009

6. Erratum: Antidepressant-like activity and modulation of brain monoaminergic transmission by blockade of anandamide hydrolysis (Proceedings of the National Academy of Sciences of the United States of America (December 20, 2005) 102, 51 (18620-18625) DOI: 10.1073/pnas.0509591102)

Author

Gobbi, G, Bambico, FR, Mangieri, R, Bortolato, M, Campolongo, P, Solinas, M, Cassano, T, Morgese, MG, Debonnel, G, Duranti, A, Tontini, A, Tarzia, G, Mor, M, Trezza, V, Goldberg, SR, Cuomo, V, and Piomelli, D

Published
2006

7. Antidepressant-like activity and modulation of brain monoaminergic transmission by blockade of anandamide hydrolysis

Author

Gobbi, G, Bambico, FR, Mangieri, R, Bortolato, M, Campolongo, P, Solinas, M, Cassano, T, Morgese, MG, Debonnel, G, Duranti, A, Tontini, A, Tarzia, G, Mor, M, Trezza, V, Goldberg, SR, Cuomo, V, and Piomelli, D

Subjects
Depression, Neurosciences, Cannabinoid Research, Substance Misuse, Drug Abuse (NIDA only), Mental Health, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Mental health, Animals, Antidepressive Agents, Arachidonic Acids, Behavior, Animal, Benzamides, Brain, Cannabinoid Receptor Agonists, Carbamates, Dronabinol, Endocannabinoids, Hydrolysis, Male, Mice, Mice, Inbred C57BL, Neurons, Norepinephrine, Polyunsaturated Alkamides, Rats, Receptors, Cannabinoid, Serotonin, depression, endocannabinoid, fatty-acid amide hydrolase, serotonin, URB597
Abstract

Although anecdotal reports suggest that cannabis may be used to alleviate symptoms of depression, the psychotropic effects and abuse liability of this drug prevent its therapeutic application. The active constituent of cannabis, delta9-tetrahydrocannabinol, acts by binding to brain CB1 cannabinoid receptors, but an alternative approach might be to develop agents that amplify the actions of endogenous cannabinoids by blocking their deactivation. Here, we show that URB597, a selective inhibitor of the enzyme fatty-acid amide hydrolase, which catalyzes the intracellular hydrolysis of the endocannabinoid anandamide, exerts potent antidepressant-like effects in the mouse tail-suspension test and the rat forced-swim test. Moreover, URB597 increases firing activity of serotonergic neurons in the dorsal raphe nucleus and noradrenergic neurons in the nucleus locus ceruleus. These actions are prevented by the CB1 antagonist rimonabant, are accompanied by increased brain anandamide levels, and are maintained upon repeated URB597 administration. Unlike direct CB1 agonists, URB597 does not exert rewarding effects in the conditioned place preference test or produce generalization to the discriminative effects of delta9-tetrahydrocannabinol in rats. The findings support a role for anandamide in mood regulation and point to fatty-acid amide hydrolase as a previously uncharacterized target for antidepressant drugs.

Published
2005

12. 3-Aminoazetidin-2-one derivatives as N-acylethanolamine acid amidase (NAAA) inhibitors suitable for systemic administration

Author

Fiasella, A, Nuzzi, A, Summa, M, Armirotti, A, Tarozzo, G, Tarzia, G, Mor, M, Bertozzi, F, Bandiera, T, and Piomelli, D

Abstract

N-Acylethanolamine acid amidase (NAAA) is a cysteine hydrolase that catalyzes the hydrolysis of endogenous lipid mediators such as palmitoylethanolamide (PEA). PEA has been shown to exert anti-inflammatory and antinociceptive effects in animals by engaging peroxisome proliferator-activated receptor α (PPAR-α). Thus, preventing PEA degradation by inhibiting NAAA may provide a novel approach for the treatment of pain and inflammatory states. Recently, 3-aminooxetan-2-one compounds were identified as a class of highly potent NAAA inhibitors. The utility of these compounds is limited, however, by their low chemical and plasma stabilities. In the present study, we synthesized and tested a series of N-(2-oxoazetidin-3-yl)amides as a novel class of NAAA inhibitors with good potency and improved physicochemical properties, suitable for systemic administration. Moreover, we elucidated the main structural features of 3-aminoazetidin-2-one derivatives that are critical for NAAA inhibition. Stability is the key: α-Amino-β-lactams were synthesized as amide derivatives, and the effect of the azetidin-2-one ring, the stereochemistry at the α-position, and the functionalization of the α-amino group were studied with regard to N-acylethanolamine acid amidase inhibitory potency and hydrolytic and plasma stability. © 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Published
2014
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13. Synthesis and structure-activity relationship (SAR) of 2-methyl-4-oxo-3- oxetanylcarbamic acid esters, a class of potent N-acylethanolamine acid amidase (NAAA) inhibitors

Author

Ponzano, S, Bertozzi, F, Mengatto, L, Dionisi, M, Armirotti, A, Romeo, E, Berteotti, A, Fiorelli, C, Tarozzo, G, Reggiani, A, Duranti, A, Tarzia, G, Mor, M, Cavalli, A, Piomelli, D, and Bandiera, T

Abstract

N-Acylethanolamine acid amidase (NAAA) is a lysosomal cysteine hydrolase involved in the degradation of saturated and monounsaturated fatty acid ethanolamides (FAEs), a family of endogenous lipid agonists of peroxisome proliferator-activated receptor-α, which include oleoylethanolamide (OEA) and palmitoylethanolamide (PEA). The β-lactone derivatives (S)-N-(2-oxo-3-oxetanyl)-3-phenylpropionamide (2) and (S)-N-(2-oxo-3-oxetanyl)- biphenyl-4-carboxamide (3) inhibit NAAA, prevent FAE hydrolysis in activated inflammatory cells, and reduce tissue reactions to pro-inflammatory stimuli. Recently, our group disclosed ARN077 (4), a potent NAAA inhibitor that is active in vivo by topical administration in rodent models of hyperalgesia and allodynia. In the present study, we investigated the structure-activity relationship (SAR) of threonine-derived β-lactone analogues of compound 4. The main results of this work were an enhancement of the inhibitory potency of β-lactone carbamate derivatives for NAAA and the identification of (4-phenylphenyl)-methyl-N-[(2S,3R)-2-methyl-4-oxo-oxetan-3-yl]carbamate (14q) as the first single-digit nanomolar inhibitor of intracellular NAAA activity (IC50 = 7 nM on both rat NAAA and human NAAA). © 2013 American Chemical Society.

Published
2013
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14. N -(2-Oxo-3-oxetanyl)carbamic acid esters as N-acylethanolamine acid amidase inhibitors: Synthesis and structure-activity and structure-property relationships

Author

Duranti, A, Tontini, A, Antonietti, F, Vacondio, F, Fioni, A, Silva, C, Lodola, A, Rivara, S, Solorzano, C, Piomelli, D, Tarzia, G, and Mor, M

Abstract

The β-lactone ring of N-(2-oxo-3-oxetanyl)amides, a class of N-acylethanolamine acid amidase (NAAA) inhibitors endowed with anti-inflammatory properties, is responsible for both NAAA inhibition and low compound stability. Here, we investigate the structure-activity and structure-property relationships for a set of known and new β-lactone derivatives, focusing on the new class of N-(2-oxo-3-oxetanyl)carbamates. Replacement of the amide group with a carbamate one led to different stereoselectivity for NAAA inhibition and higher intrinsic stability, because of the reduced level of intramolecular attack at the lactone ring. The introduction of a syn methyl at the β-position of the lactone further improved chemical stability. A tert-butyl substituent in the side chain reduced the reactivity with bovine serum albumin. (2S,3R)-2-Methyl-4-oxo-3-oxetanylcarbamic acid 5-phenylpentyl ester (27, URB913/ARN077) inhibited NAAA with good in vitro potency (IC 50 = 127 nM) and showed improved stability. It is rapidly cleaved in plasma, which supports its use for topical applications. © 2012 American Chemical Society.

Published
2012
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16. Synthesis and structure - Activity relationships of N -(2-Oxo-3-oxetanyl) amides as N -acylethanolamine-hydrolyzing acid amidase inhibitors

Author

Solorzano, C, Antonietti, F, Duranti, A, Tontini, A, Rivara, S, Lodola, A, Vacondio, F, Tarzia, G, Piomelli, D, and Mor, M

Abstract

The fatty acid ethanolamides (FAEs) are a family of bioactive lipid mediators that include the endogenous agonist of peroxisome proliferator- activated receptor-α, palmitoylethanolamide (PEA). FAEs are hydrolyzed intracellularly by either fatty acid amide hydrolase or N-acylethanolamine- hydrolyzing acid amidase (NAAA). Selective inhibition of NAAA by (S)-N-(2-oxo-3-oxetanyl)-3-phenylpropionamide [(S)-OOPP, 7a] prevents PEA degradation in mouse leukocytes and attenuates responses to proinflammatory stimuli. Starting from the structure of 7a, a series of β-lactones was prepared and tested on recombinant rat NAAA to explore structure-activity relationships (SARs) for this class of inhibitors and improve their in vitro potency. Following the hypothesis that these compounds inhibit NAAA by acylation of the catalytic cysteine, we identified several requirements for recognition at the active site and obtained new potent inhibitors. In particular, (S)-N-(2-oxo-3-oxetanyl)biphenyl-4-carboxamide (7h) was more potent than 7a at inhibiting recombinant rat NAAA activity (7a, IC50 = 420 nM; 7h, IC50 = 115 nM) in vitro and at reducing carrageenan-induced leukocyte infiltration in vivo. © 2010 American Chemical Society.

Published
2010
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19. Tandem mass spectrometric data-FAAH inhibitory activity relationships of some carbamic acid O-aryl esters

Author

Basso, E, Duranti, A, Mor, M, Piomelli, D, Tontini, A, Tarzia, G, and Traldi, P

Abstract

We have recently described a class of systemically active inhibitors of the intracellular activity of fatty acid amide hydrolase (FAAH) and traced extensive structure-activity relationships. These compounds, characterized by an N-alkyl carbamic acid O-aryl ester structure, exert potent anxiolytic-like effects in animal models. In the present study, possible relationships between mass spectrometric parameters (related to the propensity of the C(O)-O bond to be cleaved) and FAAH-inhibitory potency were tested. With this aim, a set of our products was analyzed by electrospray ionization mass spectrometry and the protonated molecules were decomposed by low-energy collisions. The experiments were performed by ion trap mass spectrometry, which led to a step-by-step energy deposition, thus favouring the lowest critical energy decomposition channels. For all compounds, breakdown curves relative to [MH]+ ions and to the fragment implying C(O)-O bond cleavage were obtained. The crossing point between these curves was related to the energetics of decomposition and the values found for the investigated compounds were linearly correlated (r 2 = 0.797) with their FAAH-inhibitory activity. This indicates that the energetics of the C(O)-O bond cleavage may be relevant in explaining FAAH inhibition. Copyright © 2004 John Wiley & Sons, Ltd.

Published
2004
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22. Synthesis and structure-activity relationships of a series of pyrrole cannabinoid receptor agonists

Author

Tarzia, G, Duranti, A, Tontini, A, Spadoni, G, Mor, M, Rivara, S, Plazzi, PV, Kathuria, S, and Piomelli, D

Subjects
lipids (amino acids, peptides, and proteins)
Abstract

We designed and synthesized a series of pyrrole derivatives with the aim of investigating the structure-activity relationship (SAR) for the binding of non-classical agonists to CB1 and CB2 cannabinoid receptors. Superposition of two pyrrole-containing cannabinoid agonists, JWH-007 and JWH-161, allowed us to identify positions 1, 3 and 4 of the pyrrole nucleus as amenable to additional investigation. We prepared the 1-alkyl-2,5-dimethyl-3,4-substituted pyrroles 10a-e, 11a-d, 17, 21, 25 and the tetrahydroindole 15, and evaluated their ability to bind to and activate cannabinoid receptors. Noteworthy in this set of compounds are the 4-bromopyrrole 11a, which has an affinity for CB1 and CB2 receptors comparable to that of well-characterized heterocyclic cannabimimetics such as Win-55,212-2; the amide 25, which, although possessing a moderate affinity for cannabinoid receptors, demonstrates that the 3-naphthoyl group, commonly present in indole and pyrrole cannabimimetics, can be substituted by alternative moieties; and compounds 10d, 11d, showing CB1 partial agonist properties. © 2003 Elsevier Ltd. All rights reserved.

Published
2003
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23. Design, synthesis, and structure - Activity relationships of alkylcarbamic acid aryl esters, a new class of fatty acid amide hydrolase inhibitors

Author

Tarzia, G, Duranti, A, Tontini, A, Piersanti, G, Mor, M, Rivara, S, Plazzi, PV, Park, C, Kathuria, S, and Piomelli, D

Abstract

Fatty acid amide hydrolase (FAAH), an intracellular serine hydrolase enzyme, participates in the deactivation of fatty acid ethanolamides such as the endogenous cannabinoid anandamide, the intestinal satiety factor oleoylethanolamide, and the peripheral analgesic and anti-inflammatory factor palmitoylethanolamide. In the present study, we report on the design, synthesis, and structure-activity relationships (SAR) of a novel class of potent, selective, and systemically active inhibitors of FAAH activity, which we have recently shown to exert potent anxiolytic-like effects in rats. These compounds are characterized by a carbamic template substituted with alkyl or aryl groups at their O- and N-termini. Most compounds inhibit FAAH, but not several other serine hydrolases, with potencies that depend on the size and shape of the substituents. Initial SAR investigations suggested that the requirements for optimal potency are a lipophilic N-alkyl substituent (such as n-butyl or cyclohexyl) and a bent O-aryl substituent. Furthermore, the carbamic group is essential for activity. A 3D-QSAR analysis on the alkylcarbamic acid aryl esters showed that the size and shape of the O-aryl moiety are correlated with FAAH inhibitory potency. A CoMSIA model was constructed, indicating that whereas the steric occupation of an area corresponding to the meta position of an O-phenyl ring improves potency, a region of low steric tolerance on the enzyme active site exists corresponding to the para position of the same ring. The bent shape of the O-aryl moieties that best fit the enzyme surface closely resembles the folded conformations observed in the complexes of unsaturated fatty acids with different proteins. URB524 (N-cyclohexylcarbamic acid biphenyl-3-yl ester, 9g) is the most potent compound of the series (IC50= 63 nM) and was therefore selected for further optimization.

Published
2003
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26. Direct B-Alkyl Suzuki−Miyaura Cross-Coupling of 2-Halopurines. Practical Synthesis of ST1535, a Potent Adenosine A2A Receptor Antagonist

Author

Patrizia Minetti, Francesca Bartoccini, Diana Celona, Giorgio Tarzia, Walter Cabri, Giovanni Piersanti, Bartoccini F, Cabri W, Celona D, Minetti P, Piersanti G, and Tarzia G

Subjects
chemistry.chemical_classification, Magnetic Resonance Spectroscopy, A2A, Receptor, Adenosine A2A, Stereochemistry, Adenine, Organic Chemistry, Antagonist, Adenosine A2A receptor, Regioselectivity, Triazoles, Combinatorial chemistry, Chemical synthesis, Adenosine receptor, chemistry, Purines, Yield (chemistry), Selectivity, Suzuky-Myaura, Alkyl
Abstract

The scope and limitations of using palladium-catalyzed cross-coupling reactions of diverse butyl metal species with two different 2-halopurines were evaluated. While tributylboranes reacted readily and regioselectively with both 2-chloro-6-dibenzylaminopurines and 2-iodo-6-chloropurines, all the other alkyl metal species were much less reactive and gave very poor yield and/or selectivity of the desired product. This protocol was applied to the synthesis of an important adenosine A(2A) receptor antagonist, ST1535.

Published
2010
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27. Potent, Metabolically stable 2-alkyl-8-(2H1,2,3-triazol-2-yl)-9H-adenines as Adenosine A2A receptor Ligand

Author

Carlo Tallarico, Patrizia Minetti, Simone Lucarini, Francesca Bartoccini, Michele Bassi, Federica Vacondio, Francesca Capocasa, Pietro Grossi, Francesco Manera, Giandomenico Brogin, Teresa Riccioni, Silvia Pace, Franco Borsini, Giorgio Tarzia, Maria Antonietta Stasi, Giovanni Piersanti, Walter Cabri, Pace S, Brogin, G., Stasi M.A., Riccioni T., Borsini F., Capocasa F., Manera F., Tallarico C., Grossi.P., Vacondio F., Bassi M., Bartoccini F., Lucarini S., Piersanti G., Tarzia G, Minetti P., and Cabri W

Subjects
Adenosine, Receptor, Adenosine A2A, Stereochemistry, Adenosine A2A receptor, Parkinson’s disease, adenosine A2a receptors, drug discovery, metabolic stability, purines, Biology, Ligands, Biochemistry, Structure-Activity Relationship, Side chain, Humans, General Pharmacology, Toxicology and Pharmaceutics, Purine metabolism, Alkyl, Pharmacology, chemistry.chemical_classification, purine, Dose-Response Relationship, Drug, Molecular Structure, Organic Chemistry, Antagonist, Metabolism, Triazoles, In vitro, adenosine A2a receptor, chemistry, Microsome, Microsomes, Liver, Molecular Medicine
Abstract

Inhibition of adenosine A2A receptors has been shown to elicit a therapeutic response in preclinical animal models of Parkinson's disease (PD). We previously identified the triazolo-9H-purine, ST1535, as a potent A(2A)R antagonist. Studies revealed that ST1535 is extensively hydroxylated at the ω-1 position of the butyl side chain. Here, we describe the synthesis and evaluation of derivatives in which the ω-1 position has been substituted (F, Me, OH) in order to block metabolism. The stability of the compounds was evaluated in human liver microsomes (HLM), and the affinity for A(2A)R was determined. Two compounds, (2-(3,3-dimethylbutyl)-9-methyl-8-(2H-1,2,3-triazol-2-yl)-9H-purin-6-amine (3 b) and 4-(6-amino-9-methyl-8-(2H-1,2,3-triazol-2-yl)-9H-purin-2-yl)-2-methylbutan-2-ol (3 c), exhibited good affinity against A(2A)R (Ki =0.4 nM and 2 nM, respectively) and high in vitro metabolic stability (89.5% and 95.3% recovery, respectively, after incubation with HLM for two hours).

Published
2015

28. Selective melatonin MT2 receptor ligands relieve neuropathic pain through modulation of brainstem descending antinociceptive pathways

Author

Serena Boccella, Giorgio Tarzia, Franco Fraschini, Stefano Comai, Sabatino Maione, Gilberto Spadoni, Annalida Bedini, Enza Palazzo, Debora Angeloni, Sergio Dominguez-Lopez, Livio Luongo, Martha Lopez-Canul, Vinicio Granados-Soto, Gabriella Gobbi, Baptiste Lacoste, Lopez Canul, M, Palazzo, Enza, Dominguez Lopez, S, Luongo, Livio, Lacoste, B, Comai, S, Angeloni, D, Fraschini, F, Boccella, S, Spadoni, G, Bedini, A, Tarzia, G, Maione, Sabatino, Granados Soto, V, Gobbi, G., Lopez Canul, Martha, Dominguez Lopez, Sergio, Lacoste, Baptiste, Comai, Stefano, Angeloni, Debora, Fraschini, Franco, Boccella, Serena, Spadoni, Gilberto, Bedini, Annalida, Tarzia, Giorgio, Granados Soto, Vinicio, and Gobbi, Gabriella

Subjects
Male, Gabapentin, medicine.drug_class, MT2 receptors, Analgesic, Pyramidal Tracts, Wistar, Periaqueductal gray, Pharmacology, Ligands, Neuropathic pain, Partial agonist, UCM924, Acetamides, medicine, Animals, Rats, Wistar, Receptor, Pain Measurement, Melatonin, Aniline Compounds, Receptor, Melatonin, MT2, Chemistry, MT2, ON/OFF cells, Nerve injury, Receptor antagonist, Rats, Anesthesiology and Pain Medicine, Nociception, Neurology, MT2 receptors,UCM924, Periaqueductal gray,ON/OFF cells,Rostral ventromedial medulla,Melatonin, Neuralgia, Neurology (clinical), Brain Stem, Rostral ventromedial medulla, medicine.symptom, Neuroscience, medicine.drug
Abstract

Neuropathic pain is an important public health problem for which only a few treatments are available. Preclinical studies show that melatonin (MLT), a neurohormone acting on MT1 and MT2 receptors, has analgesic properties, likely through MT2 receptors. Here, we determined the effects of the novel selective MLT MT2 receptor partial agonist N-{2-([3-bromophenyl]-4-fluorophenylamino)ethyl}acetamide (UCM924) in 2 neuropathic pain models in rats and examined its supraspinal mechanism of action. In rat L5-L6 spinal nerve ligation and spared nerve injury models, UCM924 (20-40 mg/kg, subcutaneously) produced a prolonged antinociceptive effect that is : (1) dose-dependent and blocked by the selective MT2 receptor antagonist 4-phenyl-2-propionamidotetralin, (2) superior to a high dose of MLT (150 mg/kg) and comparable with gabapentin (100 mg/kg), but (3) without noticeable motor coordination impairments in the rotarod test. Using double staining immunohistochemistry, we found that MT2 receptors are expressed by glutamatergic neurons in the rostral ventrolateral periaqueductal gray. Using in vivo electrophysiology combined with tail flick, we observed that microinjection of UCM924 into the ventrolateral periaqueductal gray decreased tail flick responses, depressed the firing activity of ON cells, and activated the firing of OFF cells; all effects were MT2 receptor-dependent. Altogether, these data demonstrate that selective MT2 receptor partial agonists have analgesic properties through modulation of brainstem descending antinociceptive pathways, and MT2 receptors may represent a novel target in the treatment of neuropathic pain.

Published
2015

29. Anxiolytic effects of the melatonin MT2 receptor partial agonist UCM765: Comparison with melatonin and diazepam

Author

Annalida Bedini, Silvia Rivara, Giorgio Tarzia, Stefano Comai, Rafael Ochoa-Sanchez, Gilberto Spadoni, Quentin Rainer, Franco Fraschini, Gabriella Gobbi, Marco Mor, Ochoa Sanchez, R, Rainer, Q, Comai, Stefano, Spadoni, G, Bedini, A, Rivara, S, Fraschini, F, Mor, M, Tarzia, G, and Gobbi, G.

Subjects
Male, medicine.medical_specialty, Elevated plus maze, Tetrahydronaphthalenes, medicine.drug_class, Motor Activity, Anxiety, Partial agonist, Anxiolytic, Open field, Melatonin, Rats, Sprague-Dawley, 03 medical and health sciences, Elevated plus maze test, Novelty suppressed feeding test, UCM765, 0302 clinical medicine, Internal medicine, Acetamides, medicine, Animals, Drug Interactions, Maze Learning, Biological Psychiatry, 030304 developmental biology, Pharmacology, 0303 health sciences, Aniline Compounds, Diazepam, Dose-Response Relationship, Drug, Chemistry, Receptor, Melatonin, MT2, Antagonist, Feeding Behavior, Tryptamines, Rats, Drug Partial Agonism, Disease Models, Animal, Anxiety, Elevated plus maze test, Melatonin, Novelty suppressed feeding test, UCM765, Endocrinology, Anti-Anxiety Agents, Luzindole, 030217 neurology & neurosurgery, medicine.drug
Abstract

Melatonin (MLT) is a neurohormone known to be involved in the regulation of anxiety. Most of the physiological actions of MLT in the brain are mediated by two high-affinity G-protein-coupled receptors, denoted MT(1) and MT(2). However, the particular role of these receptors in anxiety remains to be defined. Here we used a novel MT(2)-selective partial agonist, UCM765 to evaluate the involvement of MT(2) receptors in anxiety. Adult male rats were acutely injected with UCM765 (5-10-20mg/kg), MLT (20mg/kg) or diazepam (DZ, 1mg/kg). Anxiety-related behaviors were assessed in the elevated plus maze test (EPMT), novelty suppressed feeding test (NSFT) and open field test (OFT). UCM765 at the dose of 10mg/kg showed anxiolytic-like properties by increasing the time spent in the open arm of the EPMT, and by reducing the latency to eat in a novel environment in the NSFT. In the EPMT, animals treated with UCM765 (10mg/kg) or MLT (20mg/kg) spent more time in the open arms compared to vehicle-treated animals, but to a lesser extent compared to DZ (1mg/kg). In the NSFT, all treatments similarly decreased the latency to eat in a novel environment compared to vehicle. UCM765 and MLT did not affect the total time and the number of entries into the central area of the OFT, but unlike DZ, did not impair locomotion. The anxiolytic effects of UCM765 and MLT in the EPMT and the NSFT were blocked using a pre-treatment with the MT(1)/MT(2) antagonist luzindole (10mg/kg) or the MT(2) antagonist 4P-PDOT (10mg/kg). These results demonstrated, for the first time, the anxiolytic properties of UCM765 and suggest that MT(2)-receptors may be considered a novel target for the development of anxiolytic drugs.

Published
2012

30. Promotion of Non-Rapid Eye Movement Sleep and Activation of Reticular Thalamic Neurons by a Novel MT(2) Melatonin Receptor Ligand

Author

Silvia Rivara, Sergio Dominguez-Lopez, Francis Rodriguez Bambico, Baptiste Lacoste, Marco Mor, Franco Fraschini, Giorgio Tarzia, Gilberto Spadoni, Gabriella Gobbi, Laurent Descarries, Debora Angeloni, Rafael Ochoa-Sanchez, Stefano Comai, Annalida Bedini, Ochoa Sanchez, R, Comai, Stefano, Lacoste, B, Bambico, Fr, Dominguez Lopez, S, Spadoni, G, Rivara, S, Bedini, A, Angeloni, D, Fraschini, F, Mor, M, Tarzia, G, Descarries, L, and Gobbi, G.

Subjects
Male, medicine.medical_specialty, Biology, Non-rapid eye movement sleep, Partial agonist, Melatonin, Rats, Sprague-Dawley, Mice, Thalamus, Internal medicine, Acetamides, medicine, Animals, Receptor, Mice, Knockout, Neurons, Aniline Compounds, Receptor, Melatonin, MT2, General Neuroscience, Antagonist, Articles, Blockade, Rats, Endocrinology, Reticular connective tissue, Systemic administration, Female, Sleep, medicine.drug
Abstract

Melatonin activates two brain G-protein coupled receptors, MT1and MT2, whose differential roles in the sleep–wake cycle remain to be defined. The novel MT2receptor partial agonist,N-{2-[(3-methoxyphenyl) phenylamino] ethyl} acetamide (UCM765), is here shown to selectively promote non-rapid eye movement sleep (NREMS) in rats and mice. The enhancement of NREMS by UCM765 is nullified by the pharmacological blockade or genetic deletion of MT2receptors. MT2, but not MT1, knock-out mice show a decrease in NREMS compared to the wild strain. Immunohistochemical labeling reveals that MT2receptors are localized in sleep-related brain regions, and notably the reticular thalamic nucleus (Rt). Microinfusion of UCM765 in the Rt promotes NREMS, and its systemic administration induces an increase in firing and rhythmic burst activity of Rt neurons, which is blocked by the MT2antagonist 4-phenyl-2-propionamidotetralin. Since developing hypnotics that increase NREMS without altering sleep architecture remains a medical challenge, MT2receptors may represent a novel target for the treatment of sleep disorders.

Published
2011

31. Antidepressant-like activity and modulation of brain monoaminergic transmission by blockade of anandamide hydrolysis

Author

Gabriella Gobbi, Marco Bortolato, Marco Mor, Steven R. Goldberg, Vincenzo Cuomo, Marcello Solinas, Guy Debonnel, Patrizia Campolongo, Andrea Duranti, Regina A. Mangieri, Viviana Trezza, Francis Rodriguez Bambico, Maria Grazia Morgese, Andrea Tontini, Tommaso Cassano, Giorgio Tarzia, Daniele Piomelli, Institut de physiologie et biologie cellulaires (IPBC), Université de Poitiers-Centre National de la Recherche Scientifique (CNRS), Gobbi, G, Bambico, Fr, Mangieri, R, Bortolato, M, Campolongo, P, Solinas, M, Cassano, T, Morgese, Mg, Debonnel, G, Duranti, A, Tontini, A, Tarzia, G, Mor, M, Trezza, Viviana, Goldberg, Sr, Cuomo, V, and Piomelli, D.

Subjects
Male, Cannabinoid receptor, comportement, Pharmacology, chemistry.chemical_compound, Mice, Norepinephrine, 0302 clinical medicine, Rimonabant, Fatty acid amide hydrolase, Dronabinol, Receptors, Cannabinoid, PASCAL, Neurons, 0303 health sciences, Multidisciplinary, Behavior, Animal, Chemistry, Hydrolysis, Brain, Anandamide, Biological Sciences, Endocannabinoid system, Antidepressive Agents, 3. Good health, Benzamides, dépendance, medicine.drug, Serotonin, Polyunsaturated Alkamides, pharmacologie, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Arachidonic Acids, 03 medical and health sciences, Dorsal raphe nucleus, medicine, Animals, système nerveux, 030304 developmental biology, Cannabinoid Receptor Agonists, neurosciences, URB597, Conditioned place preference, Rats, Mice, Inbred C57BL, nervous system, cellule, Carbamates, depression, endocannabinoid, fatty-acid amide hydrolase, serotonin, urb597, 030217 neurology & neurosurgery, Endocannabinoids
Abstract

Although anecdotal reports suggest that cannabis may be used to alleviate symptoms of depression, the psychotropic effects and abuse liability of this drug prevent its therapeutic application. The active constituent of cannabis, Δ 9 -tetrahydrocannabinol, acts by binding to brain CB 1 cannabinoid receptors, but an alternative approach might be to develop agents that amplify the actions of endogenous cannabinoids by blocking their deactivation. Here, we show that URB597, a selective inhibitor of the enzyme fatty-acid amide hydrolase, which catalyzes the intracellular hydrolysis of the endocannabinoid anandamide, exerts potent antidepressant-like effects in the mouse tail-suspension test and the rat forced-swim test. Moreover, URB597 increases firing activity of serotonergic neurons in the dorsal raphe nucleus and noradrenergic neurons in the nucleus locus ceruleus. These actions are prevented by the CB 1 antagonist rimonabant, are accompanied by increased brain anandamide levels, and are maintained upon repeated URB597 administration. Unlike direct CB 1 agonists, URB597 does not exert rewarding effects in the conditioned place preference test or produce generalization to the discriminative effects of Δ 9 -tetrahydrocannabinol in rats. The findings support a role for anandamide in mood regulation and point to fatty-acid amide hydrolase as a previously uncharacterized target for antidepressant drugs.

Published
2005
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32. Divergent synthesis of novel 9-deazaxanthine derivatives via late-stage cross-coupling reactions

Author

Giovanni Piersanti, Marco Mor, Patrizia Minetti, Walter Cabri, Giorgio Tarzia, Francesca Bartoccini, Bartoccini F, Piersanti G, Mor M, Tarzia G, Minetti P, and Cabri W

Subjects
Aza Compounds, Halogenation, Stereochemistry, Chemistry, Organic Chemistry, Late stage, cross coupling, Biochemistry, Combinatorial chemistry, Catalysis, deazaxanthine, Coupling reaction, Xanthines, Physical and Theoretical Chemistry, Uracil, Divergent synthesis, Palladium
Abstract

A small library of 8-substituted 9-deazaxanthines has been prepared by late-stage diversification of an 8-bromo-9-deazaxanthine. By utilizing palladium-catalyzed cross-coupling reactions a single key precursor can be transformed into a variety of 8-substituted-9-deazaxanthine compounds. Three key 8-bromo-9-deazaxanthine intermediates were efficiently prepared from commercially available 6-chlorouracil in six steps.

Published
2012
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33. β-Lactones Inhibit N-acylethanolamine Acid Amidase by S-Acylation of the Catalytic N-Terminal Cysteine.

Author

Armirotti A, Romeo E, Ponzano S, Mengatto L, Dionisi M, Karacsonyi C, Bertozzi F, Garau G, Tarozzo G, Reggiani A, Bandiera T, Tarzia G, Mor M, and Piomelli D

Abstract

The cysteine amidase N-acylethanolamine acid amidase (NAAA) is a member of the N-terminal nucleophile class of enzymes and a potential target for anti-inflammatory drugs. We investigated the mechanism of inhibition of human NAAA by substituted β-lactones. We characterized pharmacologically a representative member of this class, ARN077, and showed, using high-resolution liquid chromatography-tandem mass spectrometry, that this compound forms a thioester bond with the N-terminal catalytic cysteine in human NAAA.

Published
2012
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34. Promotion of non-rapid eye movement sleep and activation of reticular thalamic neurons by a novel MT2 melatonin receptor ligand.

Author

Ochoa-Sanchez R, Comai S, Lacoste B, Bambico FR, Dominguez-Lopez S, Spadoni G, Rivara S, Bedini A, Angeloni D, Fraschini F, Mor M, Tarzia G, Descarries L, and Gobbi G

Subjects
Animals, Female, Male, Mice, Mice, Knockout, Rats, Rats, Sprague-Dawley, Receptor, Melatonin, MT2 agonists, Receptor, Melatonin, MT2 genetics, Acetamides pharmacology, Aniline Compounds pharmacology, Neurons drug effects, Receptor, Melatonin, MT2 metabolism, Sleep drug effects, Thalamus drug effects
Abstract

Melatonin activates two brain G-protein coupled receptors, MT(1) and MT(2), whose differential roles in the sleep-wake cycle remain to be defined. The novel MT(2) receptor partial agonist, N-{2-[(3-methoxyphenyl) phenylamino] ethyl} acetamide (UCM765), is here shown to selectively promote non-rapid eye movement sleep (NREMS) in rats and mice. The enhancement of NREMS by UCM765 is nullified by the pharmacological blockade or genetic deletion of MT(2) receptors. MT(2), but not MT(1), knock-out mice show a decrease in NREMS compared to the wild strain. Immunohistochemical labeling reveals that MT(2) receptors are localized in sleep-related brain regions, and notably the reticular thalamic nucleus (Rt). Microinfusion of UCM765 in the Rt promotes NREMS, and its systemic administration induces an increase in firing and rhythmic burst activity of Rt neurons, which is blocked by the MT(2) antagonist 4-phenyl-2-propionamidotetralin. Since developing hypnotics that increase NREMS without altering sleep architecture remains a medical challenge, MT(2) receptors may represent a novel target for the treatment of sleep disorders.

Published
2011
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35. Direct B-alkyl Suzuki-Miyaura cross-coupling of 2-halopurines. Practical synthesis of ST1535, a potent adenosine A2A receptor antagonist.

Author

Bartoccini F, Cabri W, Celona D, Minetti P, Piersanti G, and Tarzia G

Subjects
Adenine chemical synthesis, Adenine chemistry, Magnetic Resonance Spectroscopy, Triazoles chemistry, Adenine analogs & derivatives, Purines chemistry, Receptor, Adenosine A2A metabolism, Triazoles chemical synthesis
Abstract

The scope and limitations of using palladium-catalyzed cross-coupling reactions of diverse butyl metal species with two different 2-halopurines were evaluated. While tributylboranes reacted readily and regioselectively with both 2-chloro-6-dibenzylaminopurines and 2-iodo-6-chloropurines, all the other alkyl metal species were much less reactive and gave very poor yield and/or selectivity of the desired product. This protocol was applied to the synthesis of an important adenosine A(2A) receptor antagonist, ST1535.

Published
2010
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36. Selective N-acylethanolamine-hydrolyzing acid amidase inhibition reveals a key role for endogenous palmitoylethanolamide in inflammation.

Author

Solorzano C, Zhu C, Battista N, Astarita G, Lodola A, Rivara S, Mor M, Russo R, Maccarrone M, Antonietti F, Duranti A, Tontini A, Cuzzocrea S, Tarzia G, and Piomelli D

Subjects
Amides, Amidohydrolases metabolism, Animals, Anti-Inflammatory Agents pharmacology, Butyrates pharmacology, Carrageenan, Catalytic Domain, Cell Movement drug effects, Drug Discovery, Endocannabinoids, Ethanolamines, Mice, Mice, Inbred C57BL, Neutrophils cytology, Neutrophils drug effects, Neutrophils enzymology, PPAR alpha agonists, Phenylpropionates pharmacology, Phenylurea Compounds pharmacology, Spinal Cord Injuries enzymology, Spinal Cord Injuries pathology, Amidohydrolases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Inflammation enzymology, Inflammation pathology, Palmitic Acids metabolism
Abstract

Identifying points of control in inflammation is essential to discovering safe and effective antiinflammatory medicines. Palmitoylethanolamide (PEA) is a naturally occurring lipid amide that, when administered as a drug, inhibits inflammatory responses by engaging peroxisome proliferator-activated receptor-alpha (PPAR-alpha). PEA is preferentially hydrolyzed by the cysteine amidase N-acylethanolamine-hydrolyzing acid amidase (NAAA), which is highly expressed in macrophages. Here we report the discovery of a potent and selective NAAA inhibitor, N-[(3S)-2-oxo-3-oxetanyl]-3-phenylpropanamide [(S)-OOPP], and show that this inhibitor increases PEA levels in activated leukocytes and blunts responses induced by inflammatory stimuli both in vitro and in vivo. These effects are stereoselective, mimicked by exogenous PEA, and abolished by PPAR-alpha deletion. (S)-OOPP also attenuates inflammation and tissue damage and improves recovery of motor function in mice subjected to spinal cord trauma. The results suggest that PEA activation of PPAR-alpha in leukocytes serves as an early stop signal that contrasts the progress of inflammation. The PEA-hydrolyzing amidase NAAA may provide a previously undescribed target for antiinflammatory medicines.

Published
2009
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37. URB602 inhibits monoacylglycerol lipase and selectively blocks 2-arachidonoylglycerol degradation in intact brain slices.

Author

King AR, Duranti A, Tontini A, Rivara S, Rosengarth A, Clapper JR, Astarita G, Geaga JA, Luecke H, Mor M, Tarzia G, and Piomelli D

Subjects
Amides, Animals, Arachidonic Acids chemistry, Arachidonic Acids pharmacology, Biphenyl Compounds chemistry, Brain metabolism, Catalysis drug effects, Cerebellum drug effects, Cerebellum metabolism, Endocannabinoids, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Ethanolamines, HeLa Cells, Hippocampus drug effects, Hippocampus metabolism, Humans, Kinetics, Male, Monoacylglycerol Lipases genetics, Monoacylglycerol Lipases metabolism, Organophosphonates chemistry, Organophosphonates pharmacology, Palmitic Acids metabolism, Polyunsaturated Alkamides metabolism, Rats, Rats, Wistar, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Structure-Activity Relationship, Transfection, Arachidonic Acids metabolism, Biphenyl Compounds pharmacology, Brain drug effects, Glycerides metabolism, Monoacylglycerol Lipases antagonists & inhibitors
Abstract

The N-aryl carbamate URB602 (biphenyl-3-ylcarbamic acid cyclohexyl ester) is an inhibitor of monoacylglycerol lipase (MGL), a serine hydrolase involved in the biological deactivation of the endocannabinoid 2-arachidonoyl-sn-glycerol (2-AG). Here, we investigated the mechanism by which URB602 inhibits purified recombinant rat MGL by using a combination of biochemical and structure-activity relationship (SAR) approaches. We found that URB602 weakly inhibits recombinant MGL (IC(50) = 223 +/- 63 microM) through a rapid and noncompetitive mechanism. Dialysis experiments and SAR analyses suggest that URB602 acts through a partially reversible mechanism rather than by irreversible carbamoylation of MGL. Finally, URB602 (100 microM) elevates 2-AG levels in hippocampal slice cultures without affecting levels of other endocannabinoid-related substances. Thus, URB602 may provide a useful tool by which to investigate the physiological roles of 2-AG and explore the potential interest of MGL as a therapeutic target.

Published
2007
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38. Conformational effects in enzyme catalysis: reaction via a high energy conformation in fatty acid amide hydrolase.

Author

Lodola A, Mor M, Zurek J, Tarzia G, Piomelli D, Harvey JN, and Mulholland AJ

Subjects
Binding Sites, Computer Simulation, Energy Transfer, Enzyme Activation, Protein Binding, Protein Conformation, Structure-Activity Relationship, Amidohydrolases chemistry, Amidohydrolases ultrastructure, Models, Chemical, Models, Molecular
Abstract

Quantum mechanics/molecular mechanics and molecular dynamics simulations of fatty acid amide hydrolase show that reaction (amide hydrolysis) occurs via a distinct, high energy conformation. This unusual finding has important implications for fatty acid amide hydrolase, a key enzyme in the endocannabinoid system. These results demonstrate the importance of structural fluctuations and the need to include them in the modeling of enzyme reactions. They also show that approaches based simply on studying enzyme-substrate complexes can be misleading for understanding biochemical reactivity.

Published
2007
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39. Pharmacological profile of the selective FAAH inhibitor KDS-4103 (URB597).

Author

Piomelli D, Tarzia G, Duranti A, Tontini A, Mor M, Compton TR, Dasse O, Monaghan EP, Parrott JA, and Putman D

Subjects
Amidohydrolases chemistry, Analgesics, Animals, Anxiety drug therapy, Benzamides chemistry, Benzamides therapeutic use, Brain cytology, Cannabinoids metabolism, Carbamates chemistry, Carbamates therapeutic use, Depression drug therapy, Dose-Response Relationship, Drug, Drug Interactions, Enzyme Inhibitors chemistry, Enzyme Inhibitors therapeutic use, Humans, Pharmacokinetics, Amidohydrolases antagonists & inhibitors, Benzamides pharmacology, Carbamates pharmacology, Enzyme Inhibitors pharmacology, Neurons drug effects
Abstract

In the present article, we review the pharmacological properties of KDS-4103 (URB597), a highly potent and selective inhibitor of the enzyme fatty-acid amide hydrolase (FAAH), which catalyzes the intracellular hydrolysis of the endocannabinoid anandamide. In vitro, KDS-4103 inhibits FAAH activity with median inhibitory concentrations (IC(50)) of 5 nM in rat brain membranes and 3 nM in human liver microsomes. In vivo, KDS-4103 inhibits rat brain FAAH activity after intraperitoneal (i.p.) administration with a median inhibitory dose (ID(50)) of 0.15 mg/kg. The compound does not significantly interact with other cannabinoid-related targets, including cannabinoid receptors and anandamide transport, or with a broad panel of receptors, ion channels, transporters and enzymes. By i.p. administration to rats and mice KDS-4103 elicits significant, anxiolytic-like, antidepressant-like and analgesic effects, which are prevented by treatment with CB1 receptor antagonists. By contrast, at doses that significantly inhibit FAAH activity and substantially raise brain anandamide levels, KDS-4103 does not evoke classical cannabinoid-like effects (e.g., catalepsy, hypothermia, hyperphagia), does not cause place preference, and does not produce generalization to the discriminative effects of the active ingredient of cannabis, Delta9-tetrahydrocannabinol (Delta9-THC). These findings suggest that KDS-4103 acts by enhancing the tonic actions of anandamide on a subset of CB(1) receptors, which may normally be engaged in controlling emotions and pain. KDS-4103 is orally available in rats and cynomolgus monkeys. Sub-chronic repeated dose studies (1,500 mg/kg, per os) in these two species have not demonstrated systemic toxicity. Likewise, no toxicity was noted in bacterial cytotoxicity tests in vitro and in the Ames test. Furthermore, no deficits were observed in rats on the rotarod test after acute i.p. treatment with KDS-4103 at doses up to 5 mg/kg or in a functional observation battery after oral doses up to 1,500 mg/kg. The results suggest that KDS-4103 will offer a novel approach with a favorable therapeutic window for the treatment of anxiety, depression and pain.

Published
2006
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40. An endocannabinoid mechanism for stress-induced analgesia.

Author

Hohmann AG, Suplita RL, Bolton NM, Neely MH, Fegley D, Mangieri R, Krey JF, Walker JM, Holmes PV, Crystal JD, Duranti A, Tontini A, Mor M, Tarzia G, and Piomelli D

Subjects
Animals, Arachidonic Acids biosynthesis, Arachidonic Acids metabolism, Biological Transport drug effects, Biphenyl Compounds pharmacology, Cannabinoid Receptor Modulators biosynthesis, Glycerides biosynthesis, Glycerides metabolism, Hydrolysis drug effects, In Vitro Techniques, Male, Mesencephalon drug effects, Mesencephalon metabolism, Monoacylglycerol Lipases antagonists & inhibitors, Monoacylglycerol Lipases metabolism, Polyunsaturated Alkamides, Rats, Rats, Sprague-Dawley, Rats, Wistar, Receptor, Cannabinoid, CB1 antagonists & inhibitors, Receptor, Cannabinoid, CB1 metabolism, Analgesia, Cannabinoid Receptor Modulators metabolism, Endocannabinoids, Stress, Physiological physiopathology
Abstract

Acute stress suppresses pain by activating brain pathways that engage opioid or non-opioid mechanisms. Here we show that an opioid-independent form of this phenomenon, termed stress-induced analgesia, is mediated by the release of endogenous marijuana-like (cannabinoid) compounds in the brain. Blockade of cannabinoid CB(1) receptors in the periaqueductal grey matter of the midbrain prevents non-opioid stress-induced analgesia. In this region, stress elicits the rapid formation of two endogenous cannabinoids, the lipids 2-arachidonoylglycerol (2-AG) and anandamide. A newly developed inhibitor of the 2-AG-deactivating enzyme, monoacylglycerol lipase, selectively increases 2-AG concentrations and, when injected into the periaqueductal grey matter, enhances stress-induced analgesia in a CB1-dependent manner. Inhibitors of the anandamide-deactivating enzyme fatty-acid amide hydrolase, which selectively elevate anandamide concentrations, exert similar effects. Our results indicate that the coordinated release of 2-AG and anandamide in the periaqueductal grey matter might mediate opioid-independent stress-induced analgesia. These studies also identify monoacylglycerol lipase as a previously unrecognized therapeutic target.

Published
2005
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41. Oleylethanolamide regulates feeding and body weight through activation of the nuclear receptor PPAR-alpha.

Author

Fu J, Gaetani S, Oveisi F, Lo Verme J, Serrano A, Rodríguez De Fonseca F, Rosengarth A, Luecke H, Di Giacomo B, Tarzia G, and Piomelli D

Subjects
Animals, Appetite Depressants metabolism, Appetite Depressants pharmacology, Circadian Rhythm physiology, Gene Deletion, Gene Expression Regulation drug effects, HeLa Cells, Humans, Intestinal Mucosa metabolism, Lipid Metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Nitric Oxide Synthase genetics, Nitric Oxide Synthase Type II, Oleic Acid biosynthesis, Oleic Acid metabolism, Protein Binding, Receptors, Cytoplasmic and Nuclear agonists, Receptors, Cytoplasmic and Nuclear genetics, Transcription Factors agonists, Transcription Factors genetics, Body Weight drug effects, Feeding Behavior drug effects, Oleic Acid pharmacology, Oleic Acids, Receptors, Cytoplasmic and Nuclear metabolism, Transcription Factors metabolism
Abstract

Oleylethanolamide (OEA) is a naturally occurring lipid that regulates satiety and body weight. Although structurally related to the endogenous cannabinoid anandamide, OEA does not bind to cannabinoid receptors and its molecular targets have not been defined. Here we show that OEA binds with high affinity to the peroxisome-proliferator-activated receptor-alpha (PPAR-alpha), a nuclear receptor that regulates several aspects of lipid metabolism. Administration of OEA produces satiety and reduces body weight gain in wild-type mice, but not in mice deficient in PPAR-alpha. Two distinct PPAR-alpha agonists have similar effects that are also contingent on PPAR-alpha expression, whereas potent and selective agonists for PPAR-gamma and PPAR-beta/delta are ineffective. In the small intestine of wild-type but not PPAR-alpha-null mice, OEA regulates the expression of several PPAR-alpha target genes: it initiates the transcription of proteins involved in lipid metabolism and represses inducible nitric oxide synthase, an enzyme that may contribute to feeding stimulation. Our results, which show that OEA induces satiety by activating PPAR-alpha, identify an unexpected role for this nuclear receptor in regulating behaviour, and raise possibilities for the treatment of eating disorders.

Published
2003
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42. Modulation of anxiety through blockade of anandamide hydrolysis.

Author

Kathuria S, Gaetani S, Fegley D, Valiño F, Duranti A, Tontini A, Mor M, Tarzia G, La Rana G, Calignano A, Giustino A, Tattoli M, Palmery M, Cuomo V, and Piomelli D

Subjects
Amidohydrolases metabolism, Animals, Anti-Anxiety Agents chemistry, Anti-Anxiety Agents pharmacology, Anti-Anxiety Agents therapeutic use, Anxiety drug therapy, Arachidonic Acids therapeutic use, Behavior, Animal drug effects, Behavior, Animal physiology, Cannabinoids antagonists & inhibitors, Cannabinoids therapeutic use, Cells, Cultured, Dose-Response Relationship, Drug, Endocannabinoids, Humans, Molecular Structure, Neurons cytology, Neurons drug effects, Neurons metabolism, Piperidines pharmacology, Polyunsaturated Alkamides, Pyrazoles pharmacology, Radioligand Assay, Rats, Rats, Wistar, Receptors, Cannabinoid, Receptors, Drug metabolism, Rimonabant, Vocalization, Animal, Amidohydrolases antagonists & inhibitors, Anti-Anxiety Agents metabolism, Anxiety metabolism, Arachidonic Acids metabolism, Cannabinoids metabolism
Abstract

The psychoactive constituent of cannabis, Delta(9)-tetrahydrocannabinol, produces in humans subjective responses mediated by CB1 cannabinoid receptors, indicating that endogenous cannabinoids may contribute to the control of emotion. But the variable effects of Delta(9)-tetrahydrocannabinol obscure the interpretation of these results and limit the therapeutic potential of direct cannabinoid agonists. An alternative approach may be to develop drugs that amplify the effects of endogenous cannabinoids by preventing their inactivation. Here we describe a class of potent, selective and systemically active inhibitors of fatty acid amide hydrolase, the enzyme responsible for the degradation of the endogenous cannabinoid anandamide. Like clinically used anti-anxiety drugs, in rats the inhibitors exhibit benzodiazepine-like properties in the elevated zero-maze test and suppress isolation-induced vocalizations. These effects are accompanied by augmented brain levels of anandamide and are prevented by CB1 receptor blockade. Our results indicate that anandamide participates in the modulation of emotional states and point to fatty acid amide hydrolase inhibition as an innovative approach to anti-anxiety therapy.

Published
2003
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43. Plant-derived phenolic compounds prevent the DNA single-strand breakage and cytotoxicity induced by tert-butylhydroperoxide via an iron-chelating mechanism.

Author

Sestili P, Diamantini G, Bedini A, Cerioni L, Tommasini I, Tarzia G, and Cantoni O

Subjects
Caffeic Acids pharmacology, Catechols pharmacology, Dose-Response Relationship, Drug, Humans, Hydrogen Peroxide pharmacology, Inhibitory Concentration 50, Models, Chemical, Oxygen metabolism, Phenols pharmacology, Polymers pharmacology, Spectrophotometry, U937 Cells, Ultraviolet Rays, Chelating Agents pharmacology, DNA drug effects, DNA Damage, Flavonoids, Iron metabolism, Phenol pharmacology, Plant Extracts pharmacology, tert-Butylhydroperoxide pharmacology
Abstract

The protective effects of selected members from a series of caffeic acid esters and flavonoids were tested in various toxicity paradigms using U937 cells, previously shown to be sensitive to either iron chelators or bona fide radical scavengers or to both classes of compounds. It was found that all the protective polyphenols were active at very low concentrations and that their effects were observed only under those conditions in which iron chelators also afforded protection. Consistently, active polyphenolic compounds, unlike the inactive ones, effectively chelated iron in an in vitro system. It follows that, at least under the experimental conditions utilized in the present study, the most prominent activity of these polyphenolic compounds resides in their ability to chelate iron. Further studies revealed that the protective effects afforded by the caffeic acid esters and flavonoids were largely mediated by the catechol moiety and that the relative biological potency of these compounds was a direct function of their lipophilicity.

Published
2002
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