Melanopsin Mediates Light-dependent Relaxation in Blood Vessels

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2014 Nov 19

PMID 25404319

Citations 58

Authors

Gautam Sikka

G Patrick Hussmann

Deepesh Pandey

Suyi Cao

Daijiro Hori

Jong Taek Park

Jochen Steppan

Jae Hyung Kim

Viachaslau Barodka

Allen C Myers

Lakshmi Santhanam

Daniel Nyhan

Marc K Halushka

Raymond C Koehler

Solomon H Snyder

Larissa A Shimoda

Dan E Berkowitz

Affiliations

Soon will be listed here.

Abstract

Melanopsin (opsin4; Opn4), a non-image-forming opsin, has been linked to a number of behavioral responses to light, including circadian photo-entrainment, light suppression of activity in nocturnal animals, and alertness in diurnal animals. We report a physiological role for Opn4 in regulating blood vessel function, particularly in the context of photorelaxation. Using PCR, we demonstrate that Opn4 (a classic G protein-coupled receptor) is expressed in blood vessels. Force-tension myography demonstrates that vessels from Opn4(-/-) mice fail to display photorelaxation, which is also inhibited by an Opn4-specific small-molecule inhibitor. The vasorelaxation is wavelength-specific, with a maximal response at ∼430-460 nm. Photorelaxation does not involve endothelial-, nitric oxide-, carbon monoxide-, or cytochrome p450-derived vasoactive prostanoid signaling but is associated with vascular hyperpolarization, as shown by intracellular membrane potential measurements. Signaling is both soluble guanylyl cyclase- and phosphodiesterase 6-dependent but protein kinase G-independent. β-Adrenergic receptor kinase 1 (βARK 1 or GRK2) mediates desensitization of photorelaxation, which is greatly reduced by GRK2 inhibitors. Blue light (455 nM) regulates tail artery vasoreactivity ex vivo and tail blood blood flow in vivo, supporting a potential physiological role for this signaling system. This endogenous opsin-mediated, light-activated molecular switch for vasorelaxation might be harnessed for therapy in diseases in which altered vasoreactivity is a significant pathophysiologic contributor.

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