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糖皮质激素通过周期基因重置脉络丛的生物钟。

Glucocorticoids reset circadian clock in choroid plexus via period genes.

机构信息

Laboratory of Biological Rhythms, Institute of Physiology, Czech Academy of Sciences, Prague, Czech Republic.

Third Faculty of Medicine, Charles University, Prague, Czech Republic.

出版信息

J Endocrinol. 2021 Feb;248(2):155-166. doi: 10.1530/JOE-20-0526.

Abstract

The epithelial cells of choroid plexus (CP) in brain ventricles produce cerebrospinal fluid and act as the blood-cerebrospinal fluid barrier. In this study, we confirmed that CP in the 4th ventricle is composed of cellular oscillators that all harbor glucocorticoid receptors and are mutually synchronized to produce a robust clock gene expression rhythm detectable at the tissue level in vivo and in vitro. Animals lacking glucocorticoids (GCs) due to surgical removal of adrenal glands had Per1, Per2, Nr1d1 and Bmal1 clock gene rhythmicity in their CP significantly dampened, whereas subjecting them to daily bouts of synthetic GC analog, dexamethasone (DEX), reinforced those rhythms. We verified these in vivo effects using an in vitro model of organotypic CP explants; depending on the time of its application, DEX significantly increased the amplitude and efficiently reset the phase of the CP clock. The results are the first description of a PRC for a non-neuronal clock in the brain, demonstrating that CP clock shares some properties with the non-neuronal clocks elsewhere in the body. Finally, we found that DEX exhibited multiple synergic effects on the CP clock, including acute activation of Per1 expression and change of PER2 protein turnover rate. The DEX-induced shifts of the CP clock were partially mediated via PKA-ERK1/2 pathway. The results provide the first evidence that the GC rhythm strengthens and entrains the clock in the CP helping thus fine-tune the brain environment according to time of day.

摘要

脑室内脉络丛(CP)的上皮细胞产生脑脊液并充当血脑屏障。在这项研究中,我们证实第四脑室的 CP 由细胞振荡器组成,这些振荡器均含有糖皮质激素受体,并相互同步,以在体内和体外的组织水平上产生可检测到的强大时钟基因表达节律。由于手术切除肾上腺而缺乏糖皮质激素(GCs)的动物,其 CP 中的 Per1、Per2、Nr1d1 和 Bmal1 时钟基因节律性明显减弱,而每天给予它们合成 GC 类似物地塞米松(DEX)则增强了这些节律。我们使用 CP 器官型外植体的体外模型验证了这些体内效应;DEX 取决于其应用时间,可显著增加 CP 时钟的振幅并有效地重置其相位。这些结果首次描述了大脑中非神经元时钟的 PRC,表明 CP 时钟与身体其他部位的非神经元时钟具有一些共同特性。最后,我们发现 DEX 对 CP 时钟表现出多种协同作用,包括 Per1 表达的急性激活和 PER2 蛋白周转率的改变。DEX 诱导的 CP 时钟变化部分通过 PKA-ERK1/2 途径介导。这些结果首次提供了证据表明 GC 节律增强并使 CP 中的时钟同步,从而根据一天中的时间来微调大脑环境。

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