Your search keyword '"Gabrielle Durand"' showing total 3 results

1. The Antidepressant Metapramine is a Low-affinity Antagonist at N -methyl- d -aspartic Acid Receptors

Author

Frangoise Bordier, Adam Doble, Alain Boireau, and Gabrielle Durand

Subjects

Receptor complex, Glycine, Phencyclidine, N-Methyl-D-aspartic acid, Antidepressive Agents, Tricyclic, In Vitro Techniques, Pharmacology, Binding, Competitive, Receptors, N-Methyl-D-Aspartate, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Dibenzazepines, medicine, Animals, Receptor, Cyclic GMP, Cerebral Cortex, Binding Sites, Cell Membrane, Antagonist, Rats, Inbred Strains, Rats, chemistry, Mechanism of action, NMDA receptor, Metapramine, Dizocilpine Maleate, medicine.symptom

Abstract

Metapramine, a pharmacological compound with antidepressant activity in humans, was tested for possible antiglutamatergic activity, in vitro. We investigated the effects of metapramine on the N-methyl-d-aspartic acid (NMDA) receptor complex, by determining whether this compound would interfere with the binding of [3H]N-[1-(2-thienyl)cyclohexyl]-3,4-piperidine ([3H]TCP) to rat cortical membranes in the presence of either glycine NMDA, or both. Metapramine in the micromolar range inhibited the binding of [3H]TCP in the presence of both NMDA and glycine (ic50 = 1.4 ± 0.2 μM). That very similar affinities were observed when either NMDA or glycine was present suggests that metapramine exerted a direct action at the PCP site. The affinity of metapramine for this site was about 25 and 350 times lower than that of PCP and MK-801, respectively. Metapramine inhibited the NMDA-evoked increase in guanosine 3′,5′-cyclic monophosphate (cGMP) levels of neonatal rat cerebellar slices (ic50 = 13 μM). These results suggest that metapramine is a low-affinity antagonist of the NMDA receptor complex channel. This paper discusses the potential application of metapramine to the treatment of diseases linked to excessive stimulation of glutamatergic NMDA receptors. © 1997 Elsevier Science Ltd. All rights reserved.

Published

1996

2. Neuroprotective effects of RPR 104632, a novel antagonist at the glycine site of the NMDA receptor, in vitro

Author

Jean Marie Miquet, Marie-Claude Burgevin, M. Daniel, C. Malgouris, Mireille Meunier, Francoise Bordier, Colette Peny, Gabrielle Durand, Adam Doble, Jean-Charles Blanchard, Alain Boireau, Thierry Chevet, Serge Mignani, and Patrick Jimonet

Subjects

Stereochemistry, Phencyclidine, Guanosine, In Vitro Techniques, Pharmacology, Biology, Benzothiadiazines, Kynurenic Acid, Binding, Competitive, Hippocampus, Receptors, N-Methyl-D-Aspartate, Neuroprotection, Rats, Sprague-Dawley, chemistry.chemical_compound, stomatognathic system, medicine, Animals, Cyclic GMP, Cerebral Cortex, Antagonist, Glycine receptor antagonist, Rats, Mechanism of action, chemistry, Benzothiadiazine, Nerve Degeneration, Glycine, Aminoquinolines, NMDA receptor, medicine.symptom, Excitatory Amino Acid Antagonists

Abstract

The NMDA antagonist and neuroprotective effects of RPR 104632 (2H-1,2,4-benzothiadiazine-1-dioxide-3-carboxylic acid), a new benzothiadiazine derivative, with affinity for the glycine site of the NMDA receptor-channel complex are described. RPR 104632 antagonized the binding of [3H]5,7-dichlorokynurenic acid to the rat cerebral cortex, with a Ki of 4.9 nM. This effect was stereospecific, since the (-)-isomer was 500-fold more potent than the (+)-isomer. The potent affinity of RPR 104632 for the glycine site was confirmed by the observation that RPR 104632 inhibited [3H]N-[1-(2-thienyl)cyclohexyl]-3,4-piperidine ([3H]TCP) binding in the presence of N-methyl-D-aspartate (NMDA) (IC50 = 55 nM), whereas it had no effect on the competitive NMDA site or on the dissociative anaesthetic site. RPR 104632 inhibited the NMDA-evoked increase in guanosine 3',5'-cyclic monophosphate (cGMP) levels of neonatal rat cerebellar slices (IC50 = 890 nM) in a non-competitive manner and markedly reduced NMDA-induced neurotoxicity in rat hippocampal slices and in cortical primary cell cultures. These results suggest that RPR 104632 is a high-affinity specific antagonist of the glycine site coupled to the NMDA receptor channel with potent neuroprotective properties in vitro.

Published

1996

3. Paf binding sites

Author

Gabrielle Durand, Pierre Sedivy, Anne Floch, Daniel Pacot, Claude James, C. Robaut, Daniel Lave, Icilio Cavero, Gérard Le Fur, and S. Mondot

Subjects

Pharmacology, Lagomorpha, Platelet-activating factor, biology, Stereochemistry, Antagonist, biology.organism_classification, Ligand (biochemistry), Biochemistry, chemistry.chemical_compound, chemistry, Radioligand, Platelet, Binding site, Receptor

Abstract

52770 RP, the N -(3-chlorophenyl)-3-(3-pyridinyl)-1H, 3H-pyrrolo[1,2- c ]thiazole-7-carboxamide, displaces in a potent, specific and competitive manner [ 3 H]PAF from its binding sites on rabbit platelets. Since 52770 RP is not structurally related to PAF and has low liposolubility with respect to PAF, it was selected as a potential radioligand for PAF receptor sites. [ 3 H]52770 RP displayed high-affinity, specificity, as well as saturable and displaceable binding to a single class of recognition sites in intact platelets and crude platelet membranes. In these preparations, the values of binding parameters were, respectively, 8.5 and 7.6 nM for K d , 0.2 pmol/5 × 10 7 platelets and 3.66 pmol/mg protein for B max and 0.96 and 0.91 for nH. Inasmuch as the (+)-52770 RP was 300-fold more potent than the (−)-isomer at displacing [ 3 H]52770 RP in intact platelets, the studied binding site manifested stereospecific discrimination. A variety of pharmacological agents including pro- and anti-aggregant compounds did not exhibit affinity for [ 3 H]52770 RP binding sites. In contrast, PAF, some of its active analogues and several recognized PAF antagonists (BN 52021, brotizolam, L-652,731, triazolam), displaced the [ 3 H]52770 RP binding. Studies carried out using [ 3 H]PAF demonstrated that 52770 RP was approximately 4- and 200-fold more potent than L-652,731 and BN 52021 respectively, as a PAF-receptor antagonist. In washed rabbit platelets, the rank order of potency ( K i ) for several analogues of 52770 RP, to displace [ 3 H]PAF from its binding sites, was highly correlated ( r = 0.96) to their ability to antagonize [ 3 H]52770 RP binding. In functional studies, 52770 RP antagonized not only the PAF-induced aggregation in washed rabbit platelets but also the hypotension evoked by PAF in the anesthetized rat. In this respect, it was 26 and 2 times more potent than L-652,731, respectively. In conclusion, [ 3 H]52770 RP might represent a novel interesting tool for furthering our understanding of the role of PAF binding sites in pathophysiological processes.

Published

1987