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昼夜皮质酮的存在及相位调节雄性大鼠前额叶皮质中的时钟基因表达。

Diurnal Corticosterone Presence and Phase Modulate Clock Gene Expression in the Male Rat Prefrontal Cortex.

作者信息

Woodruff Elizabeth R, Chun Lauren E, Hinds Laura R, Spencer Robert L

机构信息

Department of Psychology and Neuroscience, University of Colorado Boulder, Boulder, Colorado 80309.

出版信息

Endocrinology. 2016 Apr;157(4):1522-34. doi: 10.1210/en.2015-1884. Epub 2016 Feb 22.

Abstract

Mood disorders are associated with dysregulation of prefrontal cortex (PFC) function, circadian rhythms, and diurnal glucocorticoid (corticosterone [CORT]) circulation. Entrainment of clock gene expression in some peripheral tissues depends on CORT. In this study, we characterized over the course of the day the mRNA expression pattern of the core clock genes Per1, Per2, and Bmal1 in the male rat PFC and suprachiasmatic nucleus (SCN) under different diurnal CORT conditions. In experiment 1, rats were left adrenal-intact (sham) or were adrenalectomized (ADX) followed by 10 daily antiphasic (opposite time of day of the endogenous CORT peak) ip injections of either vehicle or 2.5 mg/kg CORT. In experiment 2, all rats received ADX surgery followed by 13 daily injections of vehicle or CORT either antiphasic or in-phase with the endogenous CORT peak. In sham rats clock gene mRNA levels displayed a diurnal pattern of expression in the PFC and the SCN, but the phase differed between the 2 structures. ADX substantially altered clock gene expression patterns in the PFC. This alteration was normalized by in-phase CORT treatment, whereas antiphasic CORT treatment appears to have eliminated a diurnal pattern (Per1 and Bmal1) or dampened/inverted its phase (Per2). There was very little effect of CORT condition on clock gene expression in the SCN. These experiments suggest that an important component of glucocorticoid circadian physiology entails CORT regulation of the molecular clock in the PFC. Consequently, they also point to a possible mechanism that contributes to PFC disrupted function in disorders associated with abnormal CORT circulation.

摘要

情绪障碍与前额叶皮质(PFC)功能、昼夜节律以及昼夜糖皮质激素(皮质酮[CORT])循环的失调有关。某些外周组织中生物钟基因表达的同步化依赖于CORT。在本研究中,我们在一天的过程中,对处于不同昼夜CORT条件下的雄性大鼠PFC和视交叉上核(SCN)中核心生物钟基因Per1、Per2和Bmal1的mRNA表达模式进行了表征。在实验1中,大鼠保留肾上腺完整(假手术)或进行肾上腺切除(ADX),随后每天腹腔注射10次载体或2.5 mg/kg CORT(与内源性CORT峰值的时间相反)。在实验2中,所有大鼠均接受ADX手术,随后每天注射13次载体或CORT,注射时间与内源性CORT峰值相反或同步。在假手术大鼠中,生物钟基因mRNA水平在PFC和SCN中呈现出昼夜表达模式,但这两个结构之间的相位不同。ADX显著改变了PFC中生物钟基因的表达模式。这种改变通过同步CORT治疗得以正常化,而反相CORT治疗似乎消除了昼夜模式(Per1和Bmal1)或使其相位减弱/反转(Per2)。CORT条件对SCN中生物钟基因表达的影响很小。这些实验表明,糖皮质激素昼夜生理的一个重要组成部分是CORT对PFC中分子生物钟的调节。因此,它们也指出了一种可能导致与CORT循环异常相关疾病中PFC功能紊乱的机制。

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