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Satchidananda Panda,*Surendra K. Nayak,*Brice Campo,John R. Walker,John B. Hogenesch,Tim Jegla
In mammals, a small population of intrinsically photosensitiveretinal ganglion cells (ipRGCs) plays a key role in the regulationof nonvisual photic responses, such as behavioral responsesto light, pineal melatonin synthesis, pupillary light reflex,and sleep latency. These ipRGCs also express melanopsin (Opn4),a putative opsin-family photopigment that has been shown toplay a role in mediating these nonvisual photic responses. Melanopsinis required for the function of this inner retinal pathway,but its precise role in generating photic responses has notyet been determined. We found that expression of melanopsinin Xenopus oocytes results in light-dependent activation ofmembrane currents through the Gq/G11 G protein pathway, withan action spectrum closely matching that of melanopsin-expressingipRGCs and of behavioral responses to light in mice lackingrods and cones. When coexpressed with arrestins, melanopsincould use all-trans-retinaldehyde as a chromophore, which suggeststhat it may function as a bireactive opsin. We also found thatmelanopsin could activate the cation channel TRPC3, a mammalianhomolog of the Drosophila phototransduction channels TRP andTRPL. Melanopsin therefore signals more like an invertebrateopsin than like a classical vertebrate rod-and-cone opsin.
Genomics Institute of Novartis Research Foundation, 10675 John J. Hopkins Drive, San Diego, CA 92121, USA.
Note added in proof: Similar findings have recently been reported(30, 31).
* These authors contributed equally to this work.
Present address: Salk Institute for Biological Studies, La Jolla,CA 92037, USA.
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