ANTIBODIES TO A C-TERMINAL PEPTIDE OF THE RAT-BRAIN GLUTAMATE RECEPTOR SUBUNIT, GLUR-A, RECOGNIZE A SUBPOPULATION OF AMPA BINDING-SITES BUT NOT KAINATE SITES
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WENTHOLD, RJ
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机构:Section on Neurochemistry, Laboratory of Molecular Otology, National Institute on Deafness and Other Communication Disorders, Bethesda
WENTHOLD, RJ
HUNTER, C
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机构:Section on Neurochemistry, Laboratory of Molecular Otology, National Institute on Deafness and Other Communication Disorders, Bethesda
HUNTER, C
WADA, K
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机构:Section on Neurochemistry, Laboratory of Molecular Otology, National Institute on Deafness and Other Communication Disorders, Bethesda
WADA, K
DECHESNE, CJ
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机构:Section on Neurochemistry, Laboratory of Molecular Otology, National Institute on Deafness and Other Communication Disorders, Bethesda
DECHESNE, CJ
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[1] Section on Neurochemistry, Laboratory of Molecular Otology, National Institute on Deafness and Other Communication Disorders, Bethesda
Antibodies were made to a thirteen amino acid synthetic peptide corresponding to the C-terminal portion of the glutamate (glu) receptor, GluR-A. The immunoprecipitation of kainic acid (KA) and alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) binding sites by the anti-peptide antibodies was studied using a detergent-solubilized preparation of rat brain membranes. Under these conditions a subpopulation of AMPA binding sites was recognized by the antibodies, but no KA binding sites were recognized. Scatchard analysis of this subpopulation of AMPA binding sites yields a curvilinear plot which fits a two-site model with dissociation constants of 4.6 and 323 nM. These studies show that the glu receptor complex, GluR-A, binds AMPA but not KA and suggest that (i) the binding sites for these two ligands reside on different proteins, and (ii) the KA receptor identified physiologically is not equivalent to the KA binding sites identified with H-3-labelled KA.