Melanopsin phototransduction: beyond canonical cascades
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Author/Creator ORCID
Date
2021-11-29
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Citation of Original Publication
Ely Contreras, Alexis P. Nobleman, Phyllis R. Robinson, Tiffany M. Schmidt; Melanopsin phototransduction: beyond canonical cascades. J Exp Biol 1 December 2021; 224 (23): jeb226522. doi: https://doi.org/10.1242/jeb.226522
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Attribution 4.0 International (CC BY 4.0)
Attribution 4.0 International (CC BY 4.0)
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Abstract
Melanopsin is a visual pigment that is expressed in a small subset of
intrinsically photosensitive retinal ganglion cells (ipRGCs). It is
involved in regulating non-image forming visual behaviors, such as
circadian photoentrainment and the pupillary light reflex, while also
playing a role in many aspects of image-forming vision, such as
contrast sensitivity. Melanopsin was initially discovered in the
melanophores of the skin of the frog Xenopus, and subsequently
found in a subset of ganglion cells in rat, mouse and primate retinas.
ipRGCs were initially thought to be a single retinal ganglion cell
population, and melanopsin was thought to activate a single,
invertebrate-like Gq/transient receptor potential canonical (TRPC)-
based phototransduction cascade within these cells. However, in the
20 years since the discovery of melanopsin, our knowledge of this
visual pigment and ipRGCs has expanded dramatically. Six ipRGC
subtypes have now been identified in the mouse, each with unique
morphological, physiological and functional properties. Multiple
subtypes have also been identified in other species, suggesting
that this cell type diversity is a general feature of the ipRGC system.
This diversity has led to a renewed interest in melanopsin
phototransduction that may not follow the canonical Gq/TRPC
cascade in the mouse or in the plethora of other organisms that
express the melanopsin photopigment. In this Review, we discuss
recent findings and discoveries that have challenged the prevailing
view of melanopsin phototransduction as a single pathway that
influences solely non-image forming functions.