A synaptic signature for ON- and OFF-center parasol ganglion cells of the primate retina

Crook, Joanna D.; Packer, Orin S.; Dacey, Dennis M.

doi:10.1017/s0952523813000461

Cited by 55 publications

(46 citation statements)

References 93 publications

(231 reference statements)

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“…These data show that spatial integration in parasol RGC spike outputs qualitatively resembles that in the cells’ excitatory synaptic inputs (see also Crook, 2014). While there is an asymmetry in the strength of nonlinear integration in the excitatory inputs to On and Off parasol RGCs, the excitatory inputs to both cell types deviate substantially from linear spatial integration.…”

Section: Resultssupporting

confidence: 54%

Synaptic Rectification Controls Nonlinear Spatial Integration of Natural Visual Inputs

Turner

Rieke

2016

Neuron

148

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Summary A central goal in the study of any sensory system is to predict neural responses to complex inputs, especially those encountered during natural stimulation. Nowhere is the transformation from stimulus to response better understood than the vertebrate retina. Nevertheless, descriptions of retinal computation are largely based on stimulation using artificial visual stimuli, and it is unclear how these descriptions map onto the encoding of natural stimuli. We demonstrate that nonlinear spatial integration, a common feature of retinal ganglion cell (RGC) processing, shapes neural responses to natural visual stimuli in primate Off parasol RGCs, whereas On parasol RGCs exhibit surprisingly linear spatial integration. Despite this asymmetry, both cell types show strong nonlinear integration when presented with artificial stimuli. We show that nonlinear integration of natural stimuli is a consequence of rectified excitatory synaptic input, and that accounting for nonlinear spatial integration substantially improves models that predict RGC responses to natural images.

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Section: Resultssupporting

confidence: 54%

Synaptic Rectification Controls Nonlinear Spatial Integration of Natural Visual Inputs

Turner

Rieke

2016

Neuron

148

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“…2c,d) of On and Off parasol RGCs showed classical center-surround RF organization. This confirms previous observations in parasol RGCs [44,43] and other primate RGC types [45]. We then used these properties to identify a disc and annulus, matched to the specific cell, which permitted selective activation of the center or surround (Fig.…”

Section: Rf Center and Surround Interact Nonlinearly During Naturalissupporting

confidence: 66%

Receptive field center-surround interactions mediate context-dependent spatial contrast encoding in the retina

Turner

Schwartz²

2018

Preprint

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SummaryAlmost every neuron in the early visual system has some form of an antagonistic receptive field surround. But the function of the surround is poorly understood, especially under naturalistic stimulus conditions. Anatomical and functional characterization of the surround of retinal ganglion cells suggests that surround signals combine with the excitatory feedforward pathway upstream of an important synaptic nonlinearity between bipolar cells and postsynaptic ganglion cells. This circuit architecture suggests at least two unexplored consequences for receptive field structure. First, center and surround inputs should interact nonlinearly, even prior to the summation across visual space that forms the full receptive field center. Second, inputs to the surround may alter the sensitivity of the center to spatial contrast in a scene. We test these hypotheses using both synthetic and naturalistic visual stimuli, and find that the statistics of natural scenes promote these nonlinear interactions. This work shows that, unexpectedly, the surround modulates spatial contrast encoding based on visual context.

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“…The data from our study and the primate study (Crook et al . ) extend previous results by showing that synaptic NMDAR‐mediated conductances can be modulated by high temporal frequencies within the physiological range (∼10–20 Hz). The NMDAR‐mediated conductances in mammalian ganglion cells apparently are far faster than those measured in salamander ganglion cells (Mittman et al .…”

Section: Discussionsupporting

confidence: 88%

“…Our relatively fast NMDAR-mediated responses are consistent with recordings from three types of rabbit ganglion cells: postsynaptic responses to low temporal frequency stimuli exhibited NMDAR components that turned on and off rapidly and resembled the AMPAR components in time course (Venkataramani et al 2010;Buldyrev et al 2012). Furthermore, our results are consistent with recent findings from primate ganglion cells in which NMDAR-mediated conductances were recorded in response to stimulation at high temporal frequencies (Crook et al 2014). In addition, the short, ß4-9 ms delay between the peak of the AMPAR and NMDAR components of the 9-18 Hz responses that we observed (Fig.…”

Section: Broad Temporal Tuning Of Ganglion Cells Suggests That Nmdarssupporting

confidence: 93%

NMDA and AMPA receptors contribute similarly to temporal processing in mammalian retinal ganglion cells

Stafford

Manookin

Singer

et al. 2014

The Journal of Physiology

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Key pointsr In most areas of the brain, NMDA-type glutamate receptors (NMDARs) exhibit slower kinetics than do AMPA-type receptors (AMPARs).r Most retinal ganglion cells express a combination of AMPARs and NMDARs, but whether NMDAR kinetics limit temporal encoding of light stimulation is not well understood.r In this study, we measured AMPAR-and NMDAR-mediated conductances evoked by visual stimulation in two types of guinea pig retinal ganglion cell.r In both cell types, AMPAR-and NMDAR-mediated responses encoded rapidly varying contrast modulation within the physiological range (up to 18 temporal cycles s -1 ).r In retinal ganglion cells, NMDARs and AMPARs act together to encode a wide range of temporal frequencies, suggesting that NMDARs in some sensory neurons have relatively fast kinetics.Abstract Postsynaptic AMPA-and NMDA-type glutamate receptors (AMPARs, NMDARs) are commonly expressed at the same synapses. AMPARs are thought to mediate the majority of fast excitatory neurotransmission whereas NMDARs, with their relatively slower kinetics and higher Ca 2+ permeability, are thought to mediate synaptic plasticity, especially in neural circuits devoted to learning and memory. In sensory neurons, however, the roles of AMPARs and NMDARs are less well understood. Here, we tested in the in vitro guinea pig retina whether AMPARs and NMDARs differentially support temporal contrast encoding by two ganglion cell types. In both OFF Alpha and Delta ganglion cells, contrast stimulation evoked an NMDAR-mediated response with a characteristic J-shaped I-V relationship. In OFF Delta cells, AMPAR-and NMDAR-mediated responses could be modulated at low frequencies but were suppressed during 10 Hz stimulation, when responses were instead shaped by synaptic inhibition. With inhibition blocked, both AMPAR-and NMDAR-mediated responses could be modulated at 10 Hz, indicating that NMDAR kinetics do not limit temporal encoding. In OFF Alpha cells, NMDAR-mediated responses followed stimuli at frequencies up to ß18 Hz. In both cell types, NMDAR-mediated responses to contrast modulation at 9-18 Hz showed delays of <10 ms relative to AMPAR-mediated responses. Thus, NMDARs combine with AMPARs to encode rapidly modulated glutamate release, and NMDAR kinetics do not limit temporal coding by OFF Alpha and Delta ganglion cells substantially. Furthermore, glutamatergic transmission is differentially regulated across bipolar cell pathways: in some, release is suppressed at high temporal frequencies by presynaptic inhibition.

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A synaptic signature for ON- and OFF-center parasol ganglion cells of the primate retina

Cited by 55 publications

References 93 publications

Synaptic Rectification Controls Nonlinear Spatial Integration of Natural Visual Inputs

Synaptic Rectification Controls Nonlinear Spatial Integration of Natural Visual Inputs

Receptive field center-surround interactions mediate context-dependent spatial contrast encoding in the retina

NMDA and AMPA receptors contribute similarly to temporal processing in mammalian retinal ganglion cells

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