Author:
Sasaki Nobunari,Gusain Pooja,Hayano Motoshi,Sugaya Tetsuro,Tonegawa Naoya,Hatanaka Yusuke,Tamura Risako,Okuyama Kei,Osada Hideto,Ban Norimitsu,Mitsukura Yasue,Lang Richard A.,Mimura Masaru,Tsubota Kazuo
Abstract
AbstractLight stimuli from the external environment serves as a signal. Photoreceptors receive photons at the outer nuclear layer of the retina. Non-visual photoreceptors, such as opsin5 (also known as OPN5 or neuropsin), are expressed in the retinal ganglion cells (RGCs) and hypothalamus to regulate the circadian cycle and body temperature. Here, we show that violet light (VL) stimuli received by OPN5-positive RGCs are transmitted to the habenula brain region. VL improves memory in aged mice and simultaneously increases neural architecture-related genes such as oligodendrocyte-related genes in the hippocampus. In addition, VL improves depressive-like behaviors in the social defeat stress model in an OPN5 dependent manner. Following VL exposure, cFos activation is observed at the nucleus accumbens (NAc) and the paraventricular thalamic nucleus (PVT). Taken together, the results indicate that violet light modulates brain function such as memory and mood by transmitting the signal from RGCs to the habenula region in the brain.
Publisher
Cold Spring Harbor Laboratory
Cited by
4 articles.
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