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光对昼夜节律和自愿性乙醇摄入的调节:表达黑视蛋白的内在光敏性视网膜神经节细胞的作用。

Photic Regulation of Circadian Rhythms and Voluntary Ethanol Intake: Role of Melanopsin-expressing Intrinsically Photosensitive Retinal Ganglion Cells.

机构信息

Graduate School of Biomedical Science and Engineering, The University of Maine, Orono, Maine.

Department of Psychology, The University of Maine, Orono, Maine.

出版信息

J Biol Rhythms. 2021 Apr;36(2):146-159. doi: 10.1177/0748730420981228. Epub 2020 Dec 28.

Abstract

"Non-image-forming" (NIF) effects of light are mediated primarily by a subset of intrinsically photosensitive retinal ganglion cells (ipRGCs) expressing the photopigment, melanopsin (OPN4). These NIF functions include circadian entrainment, pupillary reflexes, and photic effects on sleep, mood, and cognition. We recently reported that mice of multiple genotypes exhibit reduced voluntary ethanol intake under both constant darkness (DD) and constant light (LL) relative to standard light-dark (LD) conditions. In the present study, we sought to determine whether these effects are mediated by melanopsin-expressing ipRGCs and their potential relationship to photic effects on the circadian system. To this end, we examined the effects of environmental lighting regimen on both ethanol intake and circadian activity rhythms in a genetically engineered mouse model () in which melanopsin expression is completely blocked while ipRGCs are progressively ablated due to activation of attenuated diphtheria toxin A (aDTA) transgene under the control of the promoter. As expected from previous studies, mice displayed dramatic attenuation of circadian photosensitivity, but surprisingly, showed identical suppression of ethanol intake under both DD and LL as that seen in controls. These results demonstrate that the effects of lighting regimen on voluntary ethanol intake are independent of melanopsin-expressing ipRGCs and ipRGC-mediated photic effects on the circadian system. Rather, these effects are likely mediated by classical retinal photoreceptors and central pathways.

摘要

光的“非成像”(NIF)效应主要由表达光色素黑视蛋白(OPN4)的一组固有光敏性视网膜神经节细胞(ipRGC)介导。这些 NIF 功能包括昼夜节律同步、瞳孔反射以及对睡眠、情绪和认知的光效应。我们最近报道,与标准明暗(LD)条件相比,多种基因型的小鼠在持续黑暗(DD)和持续光照(LL)下的自愿性乙醇摄入量减少。在本研究中,我们试图确定这些效应是否由表达黑视蛋白的 ipRGC 介导,以及它们与光对昼夜节律系统的潜在关系。为此,我们检查了环境光照方案对基因工程小鼠模型()中乙醇摄入和昼夜活动节律的影响,该模型中黑视蛋白表达完全被阻断,而 ipRGC 由于受启动子控制的减弱的白喉毒素 A(aDTA)转基因的激活而逐渐被消融。正如先前研究所预期的那样, 小鼠表现出昼夜光敏感性的明显衰减,但令人惊讶的是,它们在 DD 和 LL 下的乙醇摄入量抑制与对照组相同。这些结果表明,光照方案对自愿性乙醇摄入的影响独立于表达黑视蛋白的 ipRGC 和 ipRGC 对昼夜系统的光效应。相反,这些影响可能由经典的视网膜光感受器和中枢途径介导。

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