Light Affects Mood and Learning through Distinct Retina-Brain Pathways

Fernandez, Diego C.; Fogerson, P. Michelle; Ospri, Lorenzo Lazzerini; Thomsen, Michael B; Layne, Robert M.; Severín, Daniel; Zhan, Jesse; Singer, Joshua H.; Kirkwood, Alfredo; Zhao, Haiqing; Berson, David M.; Hattar, Samer

doi:10.1016/j.cell.2018.08.004

Cited by 367 publications

(344 citation statements)

References 64 publications

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“…Thus, among the areas that are innervated by the ipRGCs are the SCN, the intergeniculate leaflet (IGL), and presumably the lateral hypothalamus (LH). In previous work from another group, the acute effects of light on the brain of Arvicanthis have been reported (Shuboni et al ), showing a significant number of c‐Fos activated cells in the IGL, the LH, and the lateral habenula (LHb), or the perihabenular nucleus (PHb) in mice (Fernandez et al ). It has been previously shown that the geniculohypothalamic tract (which includes the IGL), actively modulates SCN responses to retinal input (Hanna et al ) and might modulate metabolic signals to the SCN (Saderi et al ), and reward and metabolic signals of feeding to the LHb (Huang et al ).…”

Section: Discussionmentioning

confidence: 96%

Blue light at night acutely impairs glucose tolerance and increases sugar intake in the diurnal rodent Arvicanthis ansorgei in a sex‐dependent manner

2019

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In our modern society, the exposure to light at night (LAN) has increased considerably, which may impact human health negatively. Especially exposure to light at night containing short wavelength emissions (~450–500 nm) can disrupt the normal function of the biological clock, altering sleep‐wake cycles and inducing metabolic changes. Recently, we reported that light at night acutely impairs glucose tolerance in nocturnal rats. However, light at night in nocturnal rodents coincides with their activity period, in contrast to artificial light at night exposure in humans. The aim of this study was to evaluate the acute effects of blue (λ = 490 ± 20 nm) artificial light at night (bALAN) on glucose metabolism and food intake in both male and female diurnal Sudanian grass rats (Arvicanthis ansorgei) fed either regular chow or a free choice high‐fat high sucrose diet (HFHS). In both chow and HFHS fed male Arvicanthis, 1‐hour of bALAN exposure induced a higher glucose response in the oral glucose tolerance test (OGTT) accompanied by a significant decrease in plasma insulin. Furthermore, in HFHS fed animals, bALAN induced an increase in sucrose intake during the dark phase in males but not in females. Additionally, 1‐h of bALAN increased the nonfasted glucose levels together with plasma corticosterone in female grass rats. These results provide new and further evidence for the deleterious effects of exposure to short wavelength emission‐containing artificial light at night on glucose metabolism in a diurnal rodent in a sex‐dependent manner.

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Section: Discussionmentioning

confidence: 96%

Blue light at night acutely impairs glucose tolerance and increases sugar intake in the diurnal rodent Arvicanthis ansorgei in a sex‐dependent manner

2019

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“…In nocturnal mice, an ultradian LD cycle condition induces spatial learning defects, although such an aberrant light condition does not impair the molecular clock or sleep amount (LeGates et al, 2012). The ultradian LD cycle also attenuates hippocampal long-term potentiation (Fernandez et al, 2018). In contrast, a short pulse of white light during the night before learning enhances long-lasting fear memory through the activation of hippocampal p21-activated kinase 1 (Shan et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

“…Earth’s rotation generates the daily cycle of day and night, and the rhythmic light–dark (LD) cycles have a significant impact on animal behavior and physiology. In animals, light is not only essential for acquiring information for image-forming vision in nature but also acts as a powerful modulator of brain functions such as circadian entrainment, hormone secretion, sleep-wake cycles, mood, and cognitive functions (Altimus et al, 2008; Crocker and Sehgal, 2010; Fernandez et al, 2018; LeGates et al, 2012; Vandewalle et al, 2009). Using the diurnal fruitfly Drosophila melanogaster, here, we found that LTM was severely impaired in flies kept in constant darkness (DD) after memory consolidation.…”

Section: Introductionmentioning

confidence: 99%

Environmental light is required for maintenance of long-term memory in Drosophila

Inami

Sato

Kondo³

et al. 2019

Preprint

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17 18 Long-term memory (LTM) is stored as functional modifications of relevant neural circuits 19 in the brain. However, it remains poorly understood how the consolidated memory is 20 maintained for a long period. Here, we show that in Drosophila, universally available 21 environmental light plays a critical role in LTM maintenance by reactivating the memory 22 modulator cAMP response element-binding protein (CREB) via neuropeptide signaling. 23 LTM is impaired when flies are kept in constant darkness during the memory maintenance 24 phase. Because light activates the brain neurons expressing the neuropeptide 25 Pigment-dispersing factor (Pdf) through the brain photoreceptors, we examined the 26 possible involvement of Pdf in LTM maintenance and found that temporal knockdown of 27 Pdf during the memory maintenance phase impairs LTM in light-dark cycles. Furthermore, 28 we demonstrated that the Pdf receptor (Pdfr) and CREB are required in the memory center 29 for LTM maintenance and Pdfr regulates light-dependent transcription via CREB.30 3 90When flies were kept in LL after conditioning, their LTM was intact [ Figure 1A; (7)], as previously 91 reported (Sakai et al., 2004). Furthermore, the LTM of several clock mutants except for period (per) 92 5 mutants is intact (Sakai et al., 2004). Thus, light input, but not the circadian clock, is necessary for LTM 93 maintenance. 94 Sleep plays an important role in the consolidation of Drosophila courtship memory (Donlea et al., 95 2011). However, it remains unclear whether an abnormal sleep phenotype is attributable to disturbed 96 LTM maintenance of flies kept in DD. To examine whether light conditions affect Drosophila sleep (see 97 Materials and methods), sleep amount was measured in flies kept in LD and DD (Figure 2A). The mean 98 amount of daytime sleep of flies kept in DD was lower than that of flies kept in LD (Figures 2A-C).99 However, when flies in LD were slightly deprived of sleep to adjust the amount of daytime sleep to the 100 level of that in DD (Figures 2D-F), their LTM maintenance was not attenuated (Figure 2G). Thus, LTM 101 impairment induced by DD does not simply result from the reduced amount of sleep. 102 103 Expression of brain photoreceptors in Pdf neurons is necessary for LTM maintenance in LD 104 Because light directly activates Pdf neurons through circadian photoreceptors [Rhodopsin 7 (Rh7) and 105 Cryptochrome (Cry)] (Fogle et al., 2011; Ni et al., 2017; Sheeba et al., 2008), Pdf neurons may regulate 106 light-driven LTM maintenance. To examine whether Rh7 and Cry are required for LTM, Rh7 and cry null 107 mutant flies (Rh7 1 and cry 01 , respectively) were used. Since memory on d 1 (one day after conditioning) 108 was intact in Rh7 1 and cry 01 flies after 7 h conditioning (Figure 1B), Rh7 and cry are dispensable for 109 memory consolidation. Unlike the memory on d 1, Rh7 1 and cry 01 flies showed memory impairment on d 110 5 ( Figure 1C), suggesting that Rh7 and Cry are required for keeping LTM more than one day. We next 111 sought to determin...

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“…Intriguingly, a single population of retinal projections neurons—intrinsically photosensitive retinal ganglion cells (ipRGCs)—have been implicated in the circadian and acute effects of light on many functions, including activity, sleep, and mood (Göz et al, 2008; Güler et al, 2008; Hatori et al, 2008; Legates et al, 2012; Fernandez et al, 2018). ipRGCs integrate light information from rods, cones, and their endogenous melanopsin phototransduction cascade (Schmidt et al, 2011), and relay that light information to over a dozen central targets (Hattar et al, 2006; Ecker et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

“…In comparison, the mechanisms by which ipRGCs mediate acute light responses remains largely a mystery. Genetic ablation of ipRGCs or their melanopsin phototransduction cascade blocks or attenuates the acute effects of light on sleep (Altimus et al, 2008; Lupi et al, 2008; Tsai et al, 2009), wheel-running activity (Mrosovsky and Hattar, 2003; Güler et al, 2008), and mood (Legates et al, 2012; Fernandez et al, 2018). This dual role of ipRGCs in circadian and acute light responses suggests they may share a common circuit mechanism.…”

Section: Introductionmentioning

confidence: 99%

Distinct ipRGC subpopulations mediate light's acute and circadian effects on body temperature and sleep

Rupp

Ren

Altimus

et al. 2018

Preprint

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1The light environment greatly impacts human alertness, mood, and cognition by acute 2 regulation of physiology and indirect alignment of circadian rhythms. Both processes 3 require the melanopsin-expressing intrinsically photosensitive retinal ganglion cells 4 (ipRGCs), but the relevant downstream brain areas remain elusive. ipRGCs project 5 widely in the brain, including to the central circadian pacemaker, the suprachiasmatic 6 nucleus (SCN). Here we show that body temperature and sleep responses to light are 7 absent after genetic ablation of all ipRGCs except a subpopulation that projects to the 8 SCN. Furthermore, by chemogenetic activation of the ipRGCs that avoid the SCN, we 9show that these cells are sufficient for acute changes in body temperature. Our results 10 challenge the idea that the SCN is a major relay for the acute effects of light on non-11 image forming behaviors and identify the sensory cells that initiate light's profound 12 effects on body temperature and sleep. 13 14 15 16 1 Main body

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Light Affects Mood and Learning through Distinct Retina-Brain Pathways

Cited by 367 publications

References 64 publications

Blue light at night acutely impairs glucose tolerance and increases sugar intake in the diurnal rodent Arvicanthis ansorgei in a sex‐dependent manner

Blue light at night acutely impairs glucose tolerance and increases sugar intake in the diurnal rodent Arvicanthis ansorgei in a sex‐dependent manner

Environmental light is required for maintenance of long-term memory in Drosophila

Distinct ipRGC subpopulations mediate light's acute and circadian effects on body temperature and sleep

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