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A quantitative estimate of the contribution made by various receptor categories to the depolarizations evoked by some excitatory amino acids in the olfactory cortex
Authors:GGS Collins  Gillian Brown
Institution:1. Université Grenoble Alpes, Université Savoie Mont Blanc, CNRS, IRD, IFSTAR, ISTerre, 38000 Grenoble, France.;2. Instituto de Ecología, Unidad de Calidad Ambiental (UCA), Carrera de Biología, Universidad Mayor de San Andrés, Campus Universitario de Cota Cota, casilla 3161, La Paz, Bolivia.;3. Laboratorio de Hidroquímica - Instituto de Investigaciones Químicas - Universidad Mayor de San Andrés, Campus Universitario de Cota-Cota, casilla 3161, La Paz, Bolivia.;4. Géosciences Environnement Toulouse (GET) - Institut de Recherche pour le Développement (IRD), CNRS, Université de Toulouse, France;5. Univ. Grenoble Alpes, Univ. Savoie Mont Blanc, CNRS, IRD, IFSTTAR, IGE, 38000 Grenoble, France.
Abstract:A study has been undertaken to assess the percentage contributions made by N-methyl-D-aspartate (NMDA), kainate and quisqualate receptors to the composite depolarizations evoked by L-cysteate, L-cysteinesulphinate, L-homocysteate and S-sulpho-L-cysteine in the rat olfactory cortex slice. The percentage contribution made by NMDA receptors, which was quantified by measuring the reduction in agonist responses in the presence of the highly selective NMDA receptor antagonist 2-amino-5-phosphonopentanoate (0.1 mM), was: L-homocysteate, 73%; S-sulpho-L-cysteine, 65%; L-cysteate, 42% and L-cysteinesulphinate, 30%. Responses mediated by NMDA, kainate and quisqualate receptors were abolished by a 'desensitization' procedure involving repeated application of a mixture containing high concentrations of the selective agonists followed by perfusion of the non-selective receptor antagonist cis-2,3-piperidine dicarboxylate (5 mM). Following this procedure, responses to L-homocysteate and S-sulpho-L-cysteine were almost abolished and simple calculation gave the contribution of kainate plus quisqualate receptors to the agonist responses as: L-cysteinesulphinate, 46%; L-cysteate, 34%; S-sulpho-L-cysteine, 28% and L-homocysteate, 23%. However, approximately 24% of the composite depolarizations evoked by L-cysteate and L-cysteinesulphinate was mediated by a mechanism not involving NMDA, kainate or quisqualate receptors, neither did it reflect possible electrogenic uptake of the amino acids nor an interaction with 2-amino-4-phosphonobutyrate receptors. It is suggested that this fraction of the depolarizations evoked by L-cysteate and L-cysteinesulphinate might be due to a non-receptor-mediated release of K+ or, perhaps, to activation of an as yet unidentified receptor category.
Keywords:excitatory amino acid  receptor  olfactory cortex
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