Abstract

A direct projection from melanopsin-expressing intrinsically photosensitive retinal ganglion cells (ipRGCs) reaches the primary visual thalamus (dorsal lateral geniculate nucleus; dLGN). The significance of this melanopsin input to the visual system is only recently being investigated. One unresolved question is the degree to which neurons in the dLGN could use melanopsin to track dynamic changes in light intensity under light adapted conditions. Here we set out to address this question. We were able to present full field steps visible only to melanopsin by switching between rod-isoluminant ‘yellow’ and ‘blue’ lights in a mouse lacking cone function (Cnga3-/-). In the retina these stimuli elicited melanopsin-like responses from a subset of ganglion cells. When presented to anaesthetised mice, we found that ~25-30% of visually responsive neurones in the contralateral dLGN responded to these melanopsin-isolating steps with small increases in firing rate. Such responses could be elicited even with fairly modest increases in effective irradiance (32% Michelson contrast for melanopsin). These melanopsin-driven responses were apparent at bright backgrounds (corresponding to twilight-daylight conditions), but their threshold irradiance was strongly dependent upon prior light exposure when stimuli were superimposed on a spectrally neutral ramping background light. While both onset and offset latencies were long for melanopsin-derived responses compared to those evoked by rods, there was great variability in these parameters with some cells responding to melanopsin steps in <1 s. These data indicate that a subset of dLGN units can employ melanopsin signals to detect modest changes in irradiance under photopic conditions.

Highlights

  • Photoreception in the mammalian retina is not restricted to rods and cones but extends to a population of intrinsically photosensitive retinal ganglion cells expressing the photopigment melanopsin [1, 2]

  • We found that when held under bright yellow light (12.75 log melanopsin-effective photons/cm2/sec), switches to a rod-matched blue induced modest but sustained increases in firing in 36/174 light responsive units

  • When the calibrated rod-silent, yellow-to-blue steps were presented under melanopsin-favouring conditions (30s steps against a bright background; 14.31 log melanopsin photons/cm2/s), we found measurable changes in firing rate in 54 out of 196 light responsive (LR) dLGN units from 5 animals

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Summary

Introduction

Photoreception in the mammalian retina is not restricted to rods and cones but extends to a population of intrinsically photosensitive retinal ganglion cells (ipRGCs) expressing the photopigment melanopsin [1, 2]. Accounting for

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