Sodium action potentials are not required for light-evoked release of GABA or glycine from retinal amacrine cells.

1 June 1999

journal article
research article
Published by American Physiological Society in Journal of Neurophysiology

Vol. 81 (6) , 3092-3095
https://doi.org/10.1152/jn.1999.81.6.3092

Abstract

Sodium action potentials are not required for light-evoked release of GABA or glycine from retinal amacrine cells. Although most CNS neurons require sodium action potentials (Na-APs) for normal stimulus-evoked release of classical neurotransmitters, many types of retinal and other sensory neurons instead use only graded potentials for neurotransmitter release. The physiological properties and information processing capacity of Na-AP–producing neurons appear significantly different from those of graded potential neurons. To classify amacrine cells in this dichotomy, we investigated whether Na-APs, which are often observed in these cells, are required for functional light-evoked release of inhibitory neurotransmitters from these cells. We recorded light-evoked inhibitory postsynaptic currents (IPSCs) from retinal ganglion cells, neurons directly postsynaptic to amacrine cells, and applied TTX to block Na-APs. In control solution, TTX application always led to partial suppression of the light-evoked IPSC. To isolate release from glycinergic amacrine cells, we used either bicuculline, a GABA_A receptor antagonist, or picrotoxin, a GABA_A and GABA_C receptor antagonist. TTX application only partially suppressed the glycinergic IPSC. To isolate release from GABAergic amacrine cells, we used the glycine receptor blocker strychnine. TTX application only partially suppressed the light-evoked GABAergic IPSC. Glycinergic and GABAergic amacrine cells did not obviously differ in the usage of Na-APs for release. These observations, in conjunction with previous studies of other retinal neurons, indicate that amacrine cells, taken as a class, are the only type of retinal neuron that uses both Na-AP–dependent and -independent modes for light-evoked release of neurotransmitters. These results also provide evidence for another parallel between the properties of retinal amacrine cells and olfactory bulb granule cells.

Keywords

This publication has 12 references indexed in Scilit:

Response to Change Is Facilitated by a Three-Neuron Disinhibitory Pathway in the Tiger Salamander Retina
Journal of Neuroscience, 1998
Olfactory Reciprocal Synapses: Dendritic Signaling in the CNS
Neuron, 1998
Temporal Contrast Enhancement via GABA_C Feedback at Bipolar Terminals in the Tiger Salamander Retina
Journal of Neurophysiology, 1998
Action Potentials Are Required for the Lateral Transmission of Glycinergic Transient Inhibition in the Amphibian Retina
Journal of Neuroscience, 1998
Serial inhibitory synapses in retina
Visual Neuroscience, 1997
Information processing by graded-potential transmission through tonically active synapses
Trends in Neurosciences, 1996
Effect of spike blockade on the receptive-field size of amacrine and ganglion cells in the rabbit retina
Journal of Neurophysiology, 1996
Concomitant activation of two types of glutamate receptor mediates excitation of salamander retinal ganglion cells.
The Journal of Physiology, 1990
Gated currents generate single spike activity in amacrine cells of the tiger salamander retina.
Proceedings of the National Academy of Sciences, 1986
Hyaluronidase and Retinal Function
Archives of Ophthalmology (1950), 1985