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糖皮质激素超短周期节律指导大鼠海马时钟基因周期 1 的循环基因脉冲。

Glucocorticoid ultradian rhythmicity directs cyclical gene pulsing of the clock gene period 1 in rat hippocampus.

机构信息

Henry Wellcome Laboratories for Integrative Neuroscience and Endocrinology, School of Clinical Sciences, University of Bristol, Bristol, UK.

Department of Medical Pharmacology, LACDR and Leiden University Medical Centre, The Netherlands.

出版信息

J Neuroendocrinol. 2010 Oct;22(10):1093-1100. doi: 10.1111/j.1365-2826.2010.02051.x.

Abstract

In vivo glucocorticoid (GC) secretion exhibits a distinctive ultradian rhythmicity. The lipophilic hormone can rapidly diffuse into cells, although only the pulse peak is of sufficient amplitude to activate the low affinity glucocorticoid receptor (GR). Discrete pulses readily access brain regions such as the hippocampus where GR expression is enriched and known to regulate neuronal function, including memory and learning processes. In the present study, we have tested the hypothesis that GR brain targets are responsive to ultradian GC rhythmicity. We have used adrenalectomised rats replaced with pulses of corticosterone to determine the transcriptional effects of ultradian pulses in the hippocampus. Confocal microscopy confirmed that each GC pulse results in transient GR nuclear localisation in hippocampal CA1 neurones. Concomitant GR activation and DNA binding was demonstrated by synthetic glucocorticoid response element oligonucleotide binding, and verified for the Clock gene Period 1 promoter region by chromatin immunoprecipitation assays. Strikingly each GC pulse induced a 'burst' of transcription of Period 1 measured by heterogeneous nuclear RNA quantitative polymerase chain reaction. The net effect of pulsatile GC exposure on accumulation of the mature transcript was also assessed, revealing a plateau of mRNA levels throughout the time course of pulsatile exposure, indicating the pulse timing works optimally for steady state Per1 expression. The plateau dropped to baseline within 120 min of the final pulse, indicating a relatively short half-life for hippocampal Per1. The significance of this strict temporal control is that any perturbation to the pulse frequency or duration would have rapid quantitative effects on the levels of Per1. This in turn could affect hippocampal function, especially circadian related memory and learning processes.

摘要

体内糖皮质激素(GC)的分泌表现出独特的超短周期节律性。这种亲脂性激素可以迅速扩散到细胞内,尽管只有脉冲峰值的幅度足够大,才能激活低亲和力糖皮质激素受体(GR)。离散的脉冲很容易进入富含 GR 表达的大脑区域,如海马体,GR 的表达已知可以调节神经元功能,包括记忆和学习过程。在本研究中,我们检验了以下假说,即 GR 脑靶标对超短周期 GC 节律性有反应。我们使用接受脉冲式皮质酮替代治疗的肾上腺切除术大鼠,以确定超短周期脉冲对海马体的转录影响。共聚焦显微镜证实,每个 GC 脉冲都会导致海马体 CA1 神经元中 GR 核定位的瞬时变化。通过合成糖皮质激素反应元件寡核苷酸结合证实了 GR 激活和 DNA 结合,并用染色质免疫沉淀测定法验证了 Clock 基因 Period1 启动子区域。引人注目的是,每个 GC 脉冲诱导 Period1 的转录“爆发”,通过异核 RNA 定量聚合酶链反应测量。还评估了脉冲式 GC 暴露对成熟转录物积累的净效应,结果显示在脉冲式暴露的整个时间过程中,mRNA 水平达到平台,表明脉冲定时对 Per1 的稳态表达最有效。最后一个脉冲后 120 分钟内,平台降至基线,表明海马体 Per1 的半衰期相对较短。这种严格的时间控制的意义在于,脉冲频率或持续时间的任何干扰都会对 Per1 的水平产生快速的定量影响。这反过来又会影响海马体功能,特别是与昼夜节律相关的记忆和学习过程。

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