The role of the synthetic enzyme GAD65 in the control of neuronal gamma -aminobutyric acid release

We have studied GABAergic synaptic transmission in retinal ganglion cells and hippocampal pyramidal cells to determine, at a cellular level, what is the effect of the targeted disruption of the gene encoding the synthetic enzyme GAD65 on the synaptic release of γ-aminobutyric acid (GABA). Neither the size nor the frequency of GABA-mediated spontaneous inhibitory postsynaptic currents (IPSCs) were reduced in retina or hippocampus in GAD65−/− mice. However, the release of GABA during sustained synaptic activation was substantially reduced. In the retina both electrical- and K+-induced increases in IPSC frequency were depressed without a change in IPSC amplitude. In the hippocampus the transient increase in the probability of inhibitory transmitter release associated with posttetanic potentiation was absent in the GAD65−/− mice. These results indicate that during and immediately after sustained stimulation the increase in the probability of transmitter release is not maintained in GAD65−/− mice. Such a finding suggests a decrease in the size or refilling kinetics of the releasable pool of vesicles, and various mechanisms are discussed that could account for such a defect.

The role of the synthetic enzyme GAD65 in the control of neuronal gamma -aminobutyric acid release

A bistable inhibitory optoGPCR for multiplexed optogenetic control of neural circuits

GABAergic-like dopamine synapses in the brain

Long-term plasticity induces sparse and specific synaptic changes in a biophysically detailed cortical model

A bistable inhibitory optoGPCR for multiplexed optogenetic control of neural circuits

GABAergic-like dopamine synapses in the brain

Long-term plasticity induces sparse and specific synaptic changes in a biophysically detailed cortical model