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小鼠缰核中的生物钟由儿茶酚胺设定。

The circadian clock in the mouse habenula is set by catecholamines.

机构信息

Institute of Cellular and Integrative Neurosciences, CNRS UPR-3212, 8 Allée du Général Rouvillois, Strasbourg, 67000, France.

出版信息

Cell Tissue Res. 2022 Feb;387(2):261-274. doi: 10.1007/s00441-021-03557-x. Epub 2021 Nov 24.

Abstract

Circadian rhythms are those variations in behavioral and molecular processes of organisms that follow roughly 24 h cycles in the absence of any external cue. The hypothalamic suprachiasmatic nucleus (SCN) harbors the principal brain pacemaker driving circadian rhythms. The epithalamic habenula (Hb) contains a self-sustained circadian clock functionally coupled to the SCN. Anatomically, the Hb projects to the midbrain dopamine (DA) and serotonin (5-HT) systems, and it receives inputs from the forebrain, midbrain, and brainstem. The SCN is set by internal signals such as 5-HT or melatonin from the raphe nuclei and pineal gland, respectively. However, how the Hb clock is set by internal cues is not well characterized. Hence, in the present study, we determined whether DA, noradrenaline (NA), 5-HT, and the neuropeptides orexin (ORX) and vasopressin influence the Hb circadian clock. Using PER2::Luciferase transgenic mice, we found that the amplitude of the PER2 protein circadian oscillations from Hb explants was strongly affected by DA and NA. Importantly, these effects were dose-and region (rostral vs. caudal) dependent for NA, with a main effect in the caudal part of the Hb. Furthermore, ORX also induced a significant change in the amplitude of PER2 protein oscillations in the caudal Hb. In conclusion, catecholaminergic (DA, NA) and ORXergic transmission impacts the clock properties of the Hb clock likely contributing to the circadian regulation of motivated behaviors. Accordingly, pathological conditions that lead in alterations of catecholamine or ORX activity (drug intake, compulsive feeding) might affect the Hb clock and conduct to circadian disturbances.

摘要

昼夜节律是指生物体的行为和分子过程的变化,这些变化在没有任何外部线索的情况下大致遵循 24 小时的周期。下丘脑视交叉上核 (SCN) 拥有驱动昼夜节律的主要脑起搏器。下丘脑缰核 (Hb) 包含一个自我维持的昼夜节律钟,与 SCN 功能耦合。从解剖学上讲,Hb 投射到中脑多巴胺 (DA) 和 5-羟色胺 (5-HT) 系统,并且从大脑前脑、中脑和脑干接收输入。SCN 由内部信号设置,例如来自中缝核和松果腺的 5-HT 或褪黑素。然而,Hb 时钟如何被内部线索设置还没有很好地表征。因此,在本研究中,我们确定了 DA、去甲肾上腺素 (NA)、5-HT 以及神经肽食欲素 (ORX) 和血管加压素是否影响 Hb 昼夜节律钟。使用 PER2::Luciferase 转基因小鼠,我们发现来自 Hb 外植体的 PER2 蛋白昼夜节律振荡的幅度受到 DA 和 NA 的强烈影响。重要的是,这些影响对于 NA 来说是剂量和区域(头侧与尾侧)依赖性的,在 Hb 的尾侧部分有主要作用。此外,ORX 也在 Hb 的尾侧部分显著改变了 PER2 蛋白振荡的幅度。总之,儿茶酚胺能 (DA、NA) 和 ORX 能传递影响 Hb 时钟的时钟特性,可能有助于动机行为的昼夜节律调节。因此,导致儿茶酚胺或 ORX 活性改变的病理状况(药物摄入、强迫进食)可能会影响 Hb 时钟并导致昼夜节律紊乱。

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