1. In vitro and in vivo pharmacological profile of UFP-512, a novel selective delta-opioid receptor agonist; correlations between desensitization and tolerance.
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Aguila, B., Coulbault, L., Boulouard, M., Lıveillı, F., Davis, A., Tσth, G., Borsodi, A., Balboni, G., Salvadori, S., Jauzac, P., Allouche, S., Léveillé, F, and Tóth, G
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PHARMACOLOGY , *MEDICAL sciences , *OPIOID receptors , *DESENSITIZATION (Psychotherapy) , *MENTAL depression , *ANTIDEPRESSANTS , *TRANQUILIZING drugs , *NEUROBLASTOMA , *ALLERGY desensitization , *BIOLOGICAL models , *BINDING sites , *RESEARCH , *DRUG tolerance , *MITOXANTRONE , *HETEROCYCLIC compounds , *OLIGOPEPTIDES , *ANIMAL experimentation , *RESEARCH methodology , *CELL receptors , *ANTINEOPLASTIC agents , *MEDICAL cooperation , *EVALUATION research , *DRUG administration , *CELLULAR signal transduction , *COMPARATIVE studies , *TRANSFERASES , *CYTARABINE , *SWIMMING , *ENDOCYTOSIS , *PREDNISONE , *CELL lines , *PHOSPHORYLATION , *MICE , *PHARMACODYNAMICS - Abstract
Background and Purpose: Delta-opioid receptors (DOP receptors) could represent a novel target in the treatment of depressive disorders. To explore this new field of interest, the development of highly selective DOP receptor agonists is essential. UFP-512 [H-Dmt-Tic-NH-CH(CH2-COOH)-Bid], was recently shown to behave in vitro as a selective and potent DOP receptor agonist and to promote antidepressant- and anxiolytic-like effects in vivo (Vergura et al., 2007). Here, we have characterized the pharmacological properties of UFP-512 and established a link between desensitization and tolerance.Experimental Approach: Studies were performed in the human neuroblastoma SK-N-BE cells to establish i) binding parameters for UFP-512 ii) signalling pathways activated after acute and chronic treatment iii) regulation (phosphorylation and trafficking) of human DOP (hDOP) receptors after sustained activation by UFP-512. In vivo, we studied UFP-512-induced antidepressant-like effects after acute or chronic treatment in the mouse forced swimming test.Key Results: In vitro, UFP-512 was a high affinity agonist for DOP receptors. While UFP-512 induced marked phosphorylation of DOP receptors on Ser363, we observed a low desensitization of the cAMP pathway, associated with receptor endocytosis and recycling without any reduction on extracellular signal-regulated protein kinase 1/2 activation. In vivo, acute administration of UFP-512 produced an antidepressant-like effect, without any sign of tolerance after chronic administration.Conclusions and Implications: There was a correlation between weak desensitization, significant internalization and recycling of the human DOP receptors and lack of tolerance to UFP-512. This suggests that this compound would be a promising drug prototype for exploring innovative treatments for mood disorders. [ABSTRACT FROM AUTHOR]- Published
- 2007
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