Comparing fluctuations of synaptic responses mediated via AMPA and NMDA receptor channels--implications for synaptic plasticity

Glutamate-releasing synapses are essential in fast neuronal signalling. Plasticity at these synapses is important for learning and memory as well as for the activity-dependent control of neuronal development. We have evaluated the trial-to-trial fluctuations of excitatory postsynaptic currents mediated by glutamate receptors of the AMPA and NMDA types in CA1 pyramidal cells. By using the whole cell patch clamp technique in brain slices from young rats, we have demonstrated that the relative variability of AMPA and NMDA receptor mediated responses, expressed as the coefficient of variation, is similar for these two types of responses Brain Res. 800 (1998) 253-259]. The present paper summarizes and discusses these results in relation to current theories on hippocampal synaptic plasticity, especially with regard to the ideas of glutamate spillover and silent synapses. Our finding of a correspondence between AMPA and NMDA responses with respect to fluctuations is compatible with our previous finding of equal relative changes of the two during activity induced synaptic plasticity. However, the results argue against the glutamate spillover model according to which the effect of glutamate--and hence the induction of plasticity--may spread unspecifically between synapses. But how can silent synapses become functional if no spread of glutamate occurs and no initial signal is present to trigger the functionalization? Is it necessary that NMDA responses are present at these synapses, which are then silent merely with respect to AMPA receptors, or do other alternatives exist? Our discussion aims to elucidate these questions.