RT Journal Article SR Electronic T1 Voltage-Gated Na Channels in AII Amacrine Cells Accelerate Scotopic Light Responses Mediated by the Rod Bipolar Cell Pathway JF The Journal of Neuroscience JO J. Neurosci. FD Society for Neuroscience SP 4650 OP 4659 DO 10.1523/JNEUROSCI.4212-09.2010 VO 30 IS 13 A1 Miao Tian A1 Tim Jarsky A1 Gabe J. Murphy A1 Fred Rieke A1 Joshua H. Singer YR 2010 UL http://www.jneurosci.org/content/30/13/4650.abstract AB During night (i.e., scotopic) vision in mammals, rod photoreceptor output is conveyed to ganglion cells (GCs), the output cells of the retina, by a specialized neural circuit comprising rod bipolar (RB) and AII amacrine cells. Here, we examined how intrinsic postsynaptic conductances in AIIs contribute to transmission of rod-derived signals. Using paired recordings from synaptically coupled RBs and AIIs, we found that a voltage-gated Na conductance in AII amacrines accelerated EPSPs arising from RB synaptic input. EPSPs also could be amplified by the Na conductance when AIIs were hyperpolarized below resting membrane potential, thereby increasing the availability of Na channels. AII amacrines are coupled electrically, and coupled AII amacrines likely receive common input from individual RBs. Na channel-mediated effects on EPSPs, however, appeared to occur at the single-cell rather than the AII network level. By recording light-evoked synaptic currents from GCs, we determined that the Na channel-dependent acceleration, but not amplification, of RB output by AII amacrines is reflected in the dynamics of AII synaptic output to retinal ganglion cells: synaptic inputs to both ON and OFF GCs are slowed equivalently, although not attenuated in amplitude, when Na channels in AIIs are blocked. Thus, during scotopic vision, Na conductances in AIIs serve to accelerate RB output.