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XB-ART-24050
Neuron 1992 Feb 01;82:257-65. doi: 10.1016/0896-6273(92)90292-l.
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Cloning of a putative glutamate receptor: a low affinity kainate-binding subunit.

Bettler B , Egebjerg J , Sharma G , Pecht G , Hermans-Borgmeyer I , Moll C , Stevens CF , Heinemann S .


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Kainate, a glutamate receptor agonist, is a potent neuroexcitatory agent that produces epileptiform activity and selective neuronal degeneration. Binding studies using neuronal membrane homogenates or brain sections have identified sites having either high or low affinity for [3H]kainate. Here we report the cloning of a gene, GluR7, with approximately 75% sequence identity with the previously cloned GluR5 and GluR6 subunit genes. Transcripts of the GluR7 gene are evident in brain areas that bind [3H]kainate and are susceptible to kainate-induced neurotoxicity. We have performed ligand binding studies with membranes of transfected HeLa cells expressing GluR6 or GluR7 subunits. Our data show that the GluR6 and GluR7 subunits have a rank order of agonist affinity (domoate greater than kainate much greater than L-glutamate, quisqualate much greater than AMPA, NMDA) and a dissociation constant for kainate (95 and 77 nM, respectively) characteristic of the low affinity kainate-binding sites described in the brain.

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Species referenced: Xenopus laevis
Genes referenced: grik1 grik2 grik3