Published June 16, 2023 | Version v1
Journal article Open

Mechanisms of simultaneous linear and nonlinear computations at the mammalian cone photoreceptor synapse

  • 1. University Medical Center Göttingen
  • 2. Ritsumeikan University
  • 3. Northwestern University
  • 4. University of Chicago

Description

Neurons enhance their computational power by combining linear and nonlinear transformations in extended dendritic trees. Rich, spatially distributed processing is rarely associated with individual synapses, but the cone photoreceptor synapse may be an exception. Graded voltages temporally modulate vesicle fusion at a cone's ~20 ribbon active zones. Transmitter then flows into a common, glia-free volume where bipolar cell dendrites are organized by type in successive tiers. Using super-resolution microscopy and tracking vesicle fusion and postsynaptic responses at the quantal level in the thirteen-lined ground squirrel, Ictidomys tridecemlineatus, we show that certain bipolar cell types respond to individual fusion events in the vesicle stream while other types respond to degrees of locally coincident events, creating a gradient across tiers that are increasingly nonlinear. Nonlinearities emerge from a combination of factors specific to each bipolar cell type including diffusion distance, contact number, receptor affinity, and proximity to glutamate transporters. Complex computations related to feature detection begin within the first visual synapse.

Data availability

Source data are provided with this paper for all electrophysiological traces and graphs appearing in figures. The electrophysiological traces provide a minimal basis for interpreting and verifying key results. Large image stacks (TIF) surface mesh files (STL) and associated data files are available at the Dryad repository (doi:10.5061/dryad.0p2ngf25g). Additional raw data will be shared by the corresponding author upon request. Source data are provided with this paper.

The code used to model signaling at the cone synapse is published at Zenodo and is accessible via the Dryad link at the landing page under "Related works".

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Additional details

Identifiers

DOI
10.1038/s41467-023-38943-2
Other
oai:uchicago.tind.io:6394

Related works

Funding

National Institutes of Health
R01 EY012141
JSPS KAKENHI
19H01140

UChicago Information

Division(s)
Biological Sciences Division
Department(s)
Pharmacological and Physiological Sciences