Literature DB >> 21985934

Separation of function for classical and ganglion cell photoreceptors with respect to circadian rhythm entrainment and induction of photosomnolence.

L P Morin1, K M Studholme.   

Abstract

Four studies were performed to further clarify the contribution of rod/cone and intrinsically photoreceptive retinal ganglion cells to measures of entrainment, dark preference, light-induced locomotor suppression and photosomnolence. Wild type (WT), retinally degenerate (rd/rd), and melanopsin-less (OPN4⁻/⁻) mouse strains were compared. In Experiment 1, mice were exposed to a graded photoperiod in which approximately 0.26 μW/cm² irradiance diminished to dark over a 6-h interval. This method enabled "phase angle titration," with individual animals assuming activity onsets according to their sensitivity to light. WT and OPN4⁻/⁻ animals entrained with identical phase angles (effective irradiance=0.078 μW/cm²), but rd/rd mice required a more intense irradiance (0.161 μW/cm²) and entrainment occurred about 2.5 h earlier. In Experiment 2, all three strains preferred the dark side of a divided light-dark chamber until the irradiance dropped to 0.5 μW/cm² at which point, rd/rd mice no longer showed a preference. Experiments 3 and 4 determined that WT and rd/rd mice showed equivalent light-induced locomotor suppression, but the response was greatly impaired in OPN4⁻/⁻ mice. Closer examination of open field locomotion using infrared video-based methods and Any-maze(tm) software revealed two opposing effects of light. Locomotor suppression was equivalent in WT and rd/rd mice. Responses by OPN4⁻/⁻ mice varied from being absent (n=17) to normal (similar to WT and rd/rd mice; n=8). Light onset was associated with a significant, but brief, locomotion increase in WT and OPN4⁻/⁻ mice, but not in rd/rd mice. Any-maze(tm) analysis supports the view that light-induced locomotor quiescence is followed by behavioral sleep (photosomnolence), a fact that was visually validated from the raw video files. The data show that (a) classical photoreceptors, most likely rods, allow mice to prefer and entrain to very dim light such as found in natural twilight; (b) the presence of melanopsin photopigment enables light-induced locomotor suppression and photosomnolence; (c) light-induced locomotor suppression/photosomnolence is rod/cone mediated in 36% of mice lacking melanopsin, but not in 64% of the same OPN4⁻/⁻ strain; and (d) light-induced locomotor suppression encompasses an interval of behavioral sleep.
Copyright © 2011 IBRO. Published by Elsevier Ltd. All rights reserved.

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Year:  2011        PMID: 21985934      PMCID: PMC3237860          DOI: 10.1016/j.neuroscience.2011.09.057

Source DB:  PubMed          Journal:  Neuroscience        ISSN: 0306-4522            Impact factor:   3.590


  39 in total

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2.  Absence of normal photic integration in the circadian visual system: response to millisecond light flashes.

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4.  Retinoid X receptor (gamma) is necessary to establish the S-opsin gradient in cone photoreceptors of the developing mouse retina.

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5.  Increased sexual behavior in the male rat following lesions in the mammillary region.

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6.  Differential effect of the rd mutation on rods and cones in the mouse retina.

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7.  Rod photoreceptors drive circadian photoentrainment across a wide range of light intensities.

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9.  Melanopsin and rod-cone photoreceptive systems account for all major accessory visual functions in mice.

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10.  Targeted destruction of photosensitive retinal ganglion cells with a saporin conjugate alters the effects of light on mouse circadian rhythms.

Authors:  Didem Göz; Keith Studholme; Douglas A Lappi; Mark D Rollag; Ignacio Provencio; Lawrence P Morin
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  10 in total

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2.  Brief light stimulation during the mouse nocturnal activity phase simultaneously induces a decline in core temperature and locomotor activity followed by EEG-determined sleep.

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Journal:  Am J Physiol Regul Integr Comp Physiol       Date:  2013-01-30       Impact factor: 3.619

3.  Drugs that prevent mouse sleep also block light-induced locomotor suppression, circadian rhythm phase shifts and the drop in core temperature.

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4.  Melatonin Suppression by Light in Humans Is More Sensitive Than Previously Reported.

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Review 6.  A Path to Sleep Is through the Eye

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8.  Regulation of Reentrainment Function Is Dependent on a Certain Minimal Number of Intact Functional ipRGCs in rd Mice.

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9.  Phenotype Characterization of a Mice Genetic Model of Absolute Blindness.

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10.  Effect of Intermittent versus Continuous Light Exposure on Pupillary Light Response, As Evaluated by Pupillometry.

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  10 in total

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