4.4 Article

Prolonged synaptic currents increase relay neuron firing at the developing retinogeniculate synapse

Journal

JOURNAL OF NEUROPHYSIOLOGY
Volume 112, Issue 7, Pages 1714-1728

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/jn.00451.2014

Keywords

glutamate spillover; asynchronous release; development; retinogeniculate synapse; visual system

Funding

  1. National Eye Institute (NEI) [T32 EY-007110]
  2. Childrens' Hospital Postdoctoral Career Development Fellowship
  3. PhD Training in Neuroscience National Institute of Mental Health [5T32-MH-020017]
  4. NEI [RO1-EY-013613]
  5. Children's Hospital Boston Intellectual and Developmental Disabilities Research Center National Institute of Child Health and Human Development [P01-HD-18655]

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The retinogeniculate synapse, the connection between retinal ganglion cells (RGC) and thalamic relay neurons, undergoes robust changes in connectivity over development. This process of synapse elimination and strengthening of remaining inputs is thought to require synapse specificity. Here we show that glutamate spillover and asynchronous release are prominent features of retinogeniculate synaptic transmission during this period. The immature excitatory postsynaptic currents exhibit a slow decay time course that is sensitive to low-affinity glutamate receptor antagonists and extracellular calcium concentrations, consistent with glutamate spillover. Furthermore, we uncover and characterize a novel, purely spillover-mediated AMPA receptor current from immature relay neurons. The isolation of this current strongly supports the presence of spillover between boutons of different RGCs. In addition, fluorescence measurements of presynaptic calcium transients suggest that prolonged residual calcium contributes to both glutamate spillover and asynchronous release. These data indicate that, during development, far more RGCs contribute to relay neuron firing than would be expected based on predictions from anatomy alone.

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