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Receptors, CannabinoidCannabinoid Receptor AntagonistsReceptor, Cannabinoid, CB1Receptor, Cannabinoid, CB2CannabinoidsPyrazolesCannabinoid Receptor ModulatorsPiperidinesEndocannabinoidsBornanesCannabinoid Receptor AgonistsReceptors, DrugDronabinolBenzoxazinesPolyunsaturated AlkamidesCyclohexanolsNaphthalenesArachidonic AcidsMorpholinesDose-Response Relationship, DrugRats, Sprague-DawleyGlyceridesRats, WistarCannabidiolInterleukin 1 Receptor Antagonist ProteinAnalgesicsMonoacylglycerol LipasesAmidohydrolasesNeurokinin-1 Receptor AntagonistsCannabinolCannabisExcitatory Amino Acid AntagonistsPurinergic P1 Receptor AntagonistsIndolesHistamine H2 AntagonistsSerotonin 5-HT3 Receptor AntagonistsDopamine AntagonistsRadioligand AssayAngiotensin Receptor AntagonistsAdenosine A2 Receptor AntagonistsCalcium Channel BlockersNarcotic AntagonistsLigandsNeuronsSerotonin 5-HT2 Receptor AntagonistsHormone AntagonistsBehavior, AnimalMice, Inbred C57BLDrug InteractionsSignal TransductionAdenosine A1 Receptor AntagonistsSynaptic TransmissionMice, KnockoutCapsaicinBrainCHO CellsHippocampusPurinergic P2 Receptor AntagonistsBinding, CompetitiveGuanosine 5'-O-(3-Thiotriphosphate)Histamine H1 AntagonistsCarbamatesCells, CulturedReceptors, EndothelinMuscarinic AntagonistsTRPV Cation ChannelsDrug Inverse AgonismDisease Models, AnimalReceptors, N-Methyl-D-AspartateGABA AntagonistsReceptors, Opioid, muGABA-A Receptor AntagonistsCricetinaeHistamine AntagonistsHyperalgesiaReceptors, G-Protein-CoupledSerotonin AntagonistsBenzodioxolesTime FactorsElectric StimulationPaingamma-Aminobutyric AcidGlutamic AcidSialoglycoproteinsLeukotriene AntagonistsDrug ToleranceMice, Inbred ICRReceptors, OpioidReceptor, Endothelin ARNA, MessengerEthanolaminesDizocilpine MaleateReceptors, SerotoninSerotonin 5-HT1 Receptor AntagonistsCyclohexanesMotor ActivityBiphenyl CompoundsGuinea PigsPatch-Clamp TechniquesExcitatory Postsynaptic Potentials

Rimonabant-induced Delta9-tetrahydrocannabinol withdrawal in rhesus monkeys: discriminative stimulus effects and other withdrawal signs. (73/155)

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Regulation of inflammatory pain by inhibition of fatty acid amide hydrolase. (74/155)

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Analysis of the effect of neuropeptides and cannabinoids in gastric mucosal defense initiated centrally in the rat. (75/155)

Increasing number of evidence suggest that gastric mucosal protection can be induced also centrally. Several neuropeptides, such as TRH, amylin, adrenomedullin, enkephalin, beta-endorphin, nociceptin, nocistatin, ghrelin or orexin given centrally induce gastroprotection and the dorsal vagal complex and vagal nerve may play prominent role in this centrally initiated effect. Since also cannabinoid receptors are present in the dorsal vagal complex, we aimed to study whether activation of central cannabinoid receptors result in gastric mucosal defense and whether there is an interaction between cannabinoids and endogenous opioids. Gastric mucosal damage was induced by 100% ethanol in rats. The cannabinoids were given intravenously (i.v.) or intracerebroventricularly (i.c.v.), while the antagonists were given i.c.v or intracisternally (i.c.). Gastric lesions were evaluated macroscopically 60 min later. Anandamide, methanandamide and WIN55,212-2 reduced ethanol-induced mucosal lesions after both peripheral (0.28-5.6 micromol/kg, 0.7-5.6 micromol/kg and 0.05-0.2 mumol/kg i.v., respectively) and central (2.9-115 nmol/rat, 0.27-70 nmol/rat and 1.9-38 nmol/rat i.c.v., respectively) administration. The gastroprotective effect of anandamide and methanandamide given i.c.v. or i.v.was reversed by the CB(1) receptor antagonist SR141716A (2.16 nmol i.c.v.). Naloxone (27.5 nmol i.c.v.) also antagonized the effect of i.c.v. or i.v. injected anandamide and WIN55,212-2, but less affected that of methanandamide. The gastroprotective effect of anandamide was diminished also by endomorphin-2 antiserum. In conclusion it was first demonstrated that activation of central CB(1) receptors results in gastroprotective effect. The effect is mediated at least partly by endogenous opioids.  (+info)

Rimonabant-mediated changes in intestinal lipid metabolism and improved renal vascular dysfunction in the JCR:LA-cp rat model of prediabetic metabolic syndrome. (76/155)

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Genetic deletion of fatty acid amide hydrolase alters emotional behavior and serotonergic transmission in the dorsal raphe, prefrontal cortex, and hippocampus. (77/155)

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Biochanin A, a naturally occurring inhibitor of fatty acid amide hydrolase. (78/155)

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The effect of the cannabinoid-receptor antagonist, SR141716, on the early stage of kainate-induced epileptogenesis in the adult rat. (79/155)

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2-arachidonyl glycerol activates platelets via conversion to arachidonic acid and not by direct activation of cannabinoid receptors. (80/155)

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