Hebbian induction adds AMPA-labile signaling units to CA3-CA1 synapses in the developing hippocampus

In the 2 ^nd postnatal week hippocampus, Hebbian-induced long-term potentiation (LTP) of AMPA receptor-mediated transmission in CA3-CA1 synapses is not a genuine potentiation. Instead, it is a de-depression (unsilencing) and temporary stabilization of postsynaptically AMPA-labile synapses silenced by a prior test pulse (0.03 - 0.2 Hz) stimulation. In addition to such an LTP, Hebbian induction at these synapses also results in a labile potentiation that becomes depotentiated by test pulse stimulation, thus appearing as an Hebbian-induced short- term potentiation (STP). Although the induction of this labile potentiation was blocked in the combined presence of N-methyl-D-aspartate (NMDA) and metabotropic glutamate (mGlu) receptor antagonists, the depotentiation was not affected by these drugs. The labile potentiation was not associated with a change in paired-pulse ratio and was, after a depotentiation, fully re-established by a 20 min interruption of test pulse stimulation. These properties are shared with the silencing of previously non-stimulated (naïve) AMPA-labile synapses by such test pulse stimulation. However, the depotentiation following an Hebbian induction is not a re-silencing of naïve AMPA labile synapses since there is no correlation between the magnitudes of depotentiation and preceding silencing of naïve synapses. The present results suggest that Hebbian induction at these neonatal CA3-CA1 synapses, in addition to unsilencing and temporary stabilization of AMPA-labile transmission, creates a labile potentiation based on the insertion/activation of an additional AMPA-labile signaling unit to a pre-existing synapse.