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Journal of Neuroscience, Vol 13, 1088-1096, Copyright © 1993 by Society for Neuroscience
Interactions between the glycine and glutamate binding sites of the NMDA receptor
RA Lester, G Tong and CE Jahr
Vollum Institute, Oregon Health Sciences University, Portland 97201- 3098.
The interactions between the glycine and glutamate binding sites of the
NMDA receptor have been studied in outside-out patches and synapses from
hippocampal neurons in culture using rapid drug application techniques.
Desensitization of NMDA receptor-mediated currents elicited by glutamate in
newly excised outside-out patches was reduced in the presence of saturating
concentrations of glycine. This suggests that the glutamate and glycine
binding sites of the NMDA receptor are allosterically coupled as has been
reported in whole-cell preparations. A glycine-insensitive form of
desensitization increased rapidly over the first few minutes of recording
and largely occluded the glycine concentration-sensitive desensitization in
outside-out patches. However, even in old patches that displayed no
glycine-sensitive desensitization, the unbinding rate of glycine was
increased fourfold by the presence of glutamate, suggesting that the two
binding sites were still allosterically coupled. These data suggest the
existence of two forms of NMDA receptor desensitization in outside-out
patches, only one of which is dependent on the concentration of glycine. In
the presence of saturating levels of glycine, activation of NMDA receptors
by synaptic stimulation or by exogenous glutamate resulted in currents that
relaxed biexponentially. Addition of the partial glycine-site agonist
1-hydroxy-3-aminopyrrolid-2-one (HA-966) increased the rate of decay of
both synaptic and patch currents. This suggests that HA-966 increases the
dissociation rate of glutamate from NMDA receptors. These results support
the hypothesis that the glutamate and glycine binding sites of NMDA
receptors interact allosterically; ligand binding at both types of sites
can affect the affinity of the other type for its agonist.
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