D2 dopamine receptors recruit a GABA component for their attenuation of excitatory synaptic transmission in the adult rat prefrontal cortex

Abstract

The dopamine modulation of neuronal excitability in the prefrontal cortex (PFC) changes during critical late periods of postnatal development. In particular, D₂ receptors activate fast‐spiking interneurons after, and not before, adolescence. To test the functional impact of this change, we investigated the effects of dopamine agonists on PFC excitatory synaptic transmission with whole‐cell recordings from deep‐layer pyramidal neurons in brain slices obtained from prepubertal [postnatal day (PD) 28–35] and postpubertal (PD > 51) rats. Electrical stimulation of superficial layers elicited a fast AMPA/kainate excitatory postsynaptic potential (EPSP). In the adult PFC, the D₂ agonist quinpirole decreased EPSP amplitude, an effect that lasted for at least 25 min after drug washout and was blocked by the D₂ antagonist eticlopride. The late component of this effect was blocked by the GABA‐A antagonist picrotoxin without affecting the early inhibition. Quinpirole also decreased EPSP amplitude in deep‐layer pyramidal neurons from prepubertal rats, but this response was not affected by picrotoxin. A D₁ agonist, on the other hand, did not affect the pyramidal neuron EPSP. These results indicate that D₂, not D₁, receptors attenuate local excitatory synaptic transmission in the adult PFC, and this effect of D₂ involves a recruitment of local GABAergic activity. Synapse 61:843–850, 2007.