Refinement of spatial receptive fields in the developing mouse lateral geniculate nucleus is coordinated with excitatory and inhibitory remodeling

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Abstract

Receptive field properties of individual visual neurons are dictated by the precise patterns of synaptic connections they receive, including the arrangement of inputs in visual space and features such as polarity (On vs Off). The inputs from the retina to the lateral geniculate nucleus (LGN) in the mouse undergo significant refinement during development. However, it is unknown how this refinement corresponds to the establishment of functional visual response properties. Here we conducted in vivo and in vitro recordings in the mouse LGN, beginning just after natural eye opening, to determine how receptive fields develop as excitatory and feedforward inhibitory retinal afferents refine. Experiments used both male and female subjects. For in vivo assessment of receptive fields, we performed multisite extracellular recordings in awake mice. Spatial receptive fields at eye-opening were >2 times larger than in adulthood, and decreased in size over the subsequent week. This topographic refinement was accompanied by other spatial changes, such as a decrease in spot size preference and an increase in surround suppression. Notably, the degree of specificity in terms of On/Off and sustained/transient responses appeared to be established already at eye opening and did not change. We performed in vitro recordings of the synaptic responses evoked by optic tract stimulation across the same time period. These recordings revealed a pairing of decreased excitatory and increased feedforward inhibitory convergence, providing a potential mechanism to explain the spatial receptive field refinement.

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Tschetter, W. W., Govindaiah, G., Etherington, I. M., Guido, W., & Niell, C. M. (2018). Refinement of spatial receptive fields in the developing mouse lateral geniculate nucleus is coordinated with excitatory and inhibitory remodeling. Journal of Neuroscience, 38(19), 4531–4542. https://doi.org/10.1523/JNEUROSCI.2857-17.2018

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