Abstract

Our long term goal is to understand the functional architecture of neural circuits in cat retina. Here we focus on the cone circuits to on-beta (X) and on-alpha (Y) ganglion cells. These types (with their off counterparts) account for greater that 90% of the optic nerve cross- section and divide spatio-temporal frequency space. Beta cells (narrow field, densely distributed) serve higher spatial and lower temporal frequencies; alpha cells (wide field, sparsely distributed) serve the reverse. Thus far, we have determined for both types the complete sets of parallel bipolar circuits that connect them to rods and cones. This has led to specific hypotheses regarding the basis for receptive field structure at different luminances. We now propose: 1) Complete the structure of the beta circuit. Determine amacrine cell types that supply the last 60 unidentified synapses; quantitate cone contacts to the three bipolar types with input to the beta cell (intracellular filling + confocal and electron microscopy). 2) Probe function at outer plexiform by localizing molecules that serve GABA and glutamate transmission. For GABA, localize the synthetic enzyme, transporter, and specific subunits of the GABAA receptor. For glutamate, localize (in on bipolar cells) components of G protein system possibly corresponding to the phototransduction cascade: transducins, phosphodiesterase, arrestins, cGMP ion channels (immuno- and in situ hybridization histochemistry). 3) Determine how known circuit gains for alpha and beta relate to the number of bipolar-to-ganglion cell synapses per retinal area. Measure bipolar synapses/ganglion cell membrane area at different eccentricities (EM) and dendritic membrane area/retinal area (fill + confocal). 4) Determine how the unique 3-D architectures of the alpha and beta dendritic meshworks are accounted for by known functional constraints (such as density, coverage, membrane area/retinal area, dendritic volume) and constraints on dendritic spacing. Quantitate these factors (fill neighbors of same type, confocal + 3-D graphics). 5) Assess how identified factors (optical + neural) account for beta ganglion cell performance. Construct compartmental models and ideal observer models; compare these to actual performance; assess which factors contribute to the difference. The proposed studies address fundamental mechanisms responsible for """"""""image processing"""""""" by identified circuits in mammalian brain. These studies will help to understand human retina because many features of retinal organization are shared across species.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
2R01EY000828-26
Application #
2019379
Study Section
Visual Sciences C Study Section (VISC)
Project Start
1977-04-01
Project End
2002-03-31
Budget Start
1997-04-01
Budget End
1998-03-31
Support Year
26
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Pediatrics
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Borghuis, Bart G; Sterling, Peter; Smith, Robert G (2009) Loss of sensitivity in an analog neural circuit. J Neurosci 29:3045-58
Borghuis, Bart G; Ratliff, Charles P; Smith, Robert G et al. (2008) Design of a neuronal array. J Neurosci 28:3178-89
Xu, Ying; Vasudeva, Viren; Vardi, Noga et al. (2008) Different types of ganglion cell share a synaptic pattern. J Comp Neurol 507:1871-8
Beaudoin, Deborah L; Borghuis, Bart G; Demb, Jonathan B (2007) Cellular basis for contrast gain control over the receptive field center of mammalian retinal ganglion cells. J Neurosci 27:2636-45
Zaghloul, Kareem A; Manookin, Michael B; Borghuis, Bart G et al. (2007) Functional circuitry for peripheral suppression in Mammalian Y-type retinal ganglion cells. J Neurophysiol 97:4327-40
Sterling, Peter; Freed, Michael (2007) How robust is a neural circuit? Vis Neurosci 24:563-71
Xu, Ying; Dhingra, Narender K; Smith, Robert G et al. (2005) Sluggish and brisk ganglion cells detect contrast with similar sensitivity. J Neurophysiol 93:2388-95
Zaghloul, Kareem A; Boahen, Kwabena; Demb, Jonathan B (2005) Contrast adaptation in subthreshold and spiking responses of mammalian Y-type retinal ganglion cells. J Neurosci 25:860-8
Sterling, Peter; Matthews, Gary (2005) Structure and function of ribbon synapses. Trends Neurosci 28:20-9
Choi, Sue-Yeon; Borghuis, Bart G; Borghuis, Bart et al. (2005) Encoding light intensity by the cone photoreceptor synapse. Neuron 48:555-62

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