Literature DB >> 18832424

Distinct expressions of contrast gain control in parallel synaptic pathways converging on a retinal ganglion cell.

Deborah Langrill Beaudoin1, Michael B Manookin, Jonathan B Demb.   

Abstract

Visual neurons adapt to increases in stimulus contrast by reducing their response sensitivity and decreasing their integration time, a collective process known as 'contrast gain control.' In retinal ganglion cells, gain control arises at two stages: an intrinsic mechanism related to spike generation, and a synaptic mechanism in retinal pathways. Here, we tested whether gain control is expressed similarly by three synaptic pathways that converge on an OFF alpha/Y-type ganglion cell: excitatory inputs driven by OFF cone bipolar cells; inhibitory inputs driven by ON cone bipolar cells; and inhibitory inputs driven by rod bipolar cells. We made whole-cell recordings of membrane current in guinea pig ganglion cells in vitro. At high contrast, OFF bipolar cell-mediated excitatory input reduced gain and shortened integration time. Inhibitory input was measured by clamping voltage near 0 mV or by recording in the presence of ionotropic glutamate receptor (iGluR) antagonists to isolate the following circuit: cone --> ON cone bipolar cell --> AII amacrine cell --> OFF ganglion cell. At high contrast, this input reduced gain with no effect on integration time. Mean luminance was reduced 1000-fold to recruit the rod bipolar pathway: rod --> rod bipolar cell --> AII cell --> OFF ganglion cell. The spiking response, measured with loose-patch recording, adapted despite essentially no gain control in synaptic currents. Thus, cone bipolar-driven pathways adapt differently, with kinetic effects confined to the excitatory OFF pathway. The ON bipolar-mediated inhibition reduced gain at high contrast by a mechanism that did not require an iGluR. Under rod bipolar-driven conditions, ganglion cell firing showed gain control that was explained primarily by an intrinsic property.

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Year:  2008        PMID: 18832424      PMCID: PMC2655385          DOI: 10.1113/jphysiol.2008.156224

Source DB:  PubMed          Journal:  J Physiol        ISSN: 0022-3751            Impact factor:   5.182


  67 in total

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  27 in total

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3.  Light adaptation alters the source of inhibition to the mouse retinal OFF pathway.

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4.  Synaptic noise is an information bottleneck in the inner retina during dynamic visual stimulation.

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5.  The neural circuit mechanisms underlying the retinal response to motion reversal.

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6.  NMDA receptor contributions to visual contrast coding.

Authors:  Michael B Manookin; Michael Weick; Benjamin K Stafford; Jonathan B Demb
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7.  Inferring synaptic inputs from spikes with a conductance-based neural encoding model.

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8.  Integrative properties of retinal ganglion cell electrical responsiveness depend on neurotrophic support and genotype in the mouse.

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10.  Selective synaptic connections in the retinal pathway for night vision.

Authors:  Deborah L Beaudoin; Mania Kupershtok; Jonathan B Demb
Journal:  J Comp Neurol       Date:  2017-09-15       Impact factor: 3.215

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