重复性轻度创伤性脑损伤改变青少年大鼠中枢和外周时钟基因表达

Marissa Sgro , Susanne Ellens , Zoe N. Kodila , Jennaya Christensen , Crystal Li , Richelle Mychasiuk , Glenn R. Yamakawa
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引用次数: 1

摘要

轻度创伤性脑损伤(mTBI)或脑震荡是世界范围内常见的损伤,导致高昂的医疗费用和社会负担。在青少年中,跌倒和运动相关的创伤通常是mTBI的原因。重要的是,关键的大脑生长和发育发生在这一敏感时期,这使得脑损伤的前景令人担忧。超过70%的患者报告说,这些损伤后昼夜节律紊乱,这已被证明会阻碍康复。因此,我们试图确定重复mTBI(RmTBI)大鼠模型中核心昼夜节律时钟基因表达是否被破坏。雄性和雌性青春期大鼠(n=129)接受假手术或RmTBI。然后,在白天和晚上的不同时间对这些动物实施安乐死。评估下丘脑、小脑、海马、肝脏和小肠组织中per1、per2、cry1、clock、bmal1和rev-erb-α的表达。我们发现,大多数时钟基因在昼夜之间变化,表明昼夜节律的表达模式。在下丘脑中,我们发现RmTBI改变了cry1和bmal1的表达,此外还改变了per2、cry1、clock、bmal1和rev-erb-α的性别差异。在小脑中,除了cry1、clock和bmal1表达的性别差异外,per1、per2、cry1,clock、bmal1和rev-erb-α节律都被RmTBI敲除。我们还检测到,男性在半夜所有时钟基因的总体表达都显著下降。在海马中,我们发现RmTBI除了改变bmal1表达的性别差异外,还改变了rev-erb-α表达的节律。在肝脏中,我们在所有检查的基因中都检测到了强烈的节律,然而只有per2的表达被RmTBI敲除,此外,我们还检测到per2和cry1的性别差异。我们还发现,女性时钟基因表达在深夜总体上有所下降。在小肠中,RmTBI改变了cry1的表达,并且rev-erb-α存在性别差异。这些结果表明,RmTBI以时间、组织和性别依赖的方式改变了中枢和外周神经系统中的核心昼夜节律时钟基因表达。这可能会破坏大脑和外周神经系统之间的重要阶段关系,有助于损伤后的症状学,也突出了对损伤结果进行时间和性别依赖性评估的重要性。
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Repetitive mild traumatic brain injury alters central and peripheral clock gene expression in the adolescent rat

Mild traumatic brain injury (mTBI) or concussion is a common injury worldwide leading to substantial medical costs and a high burden on society. In adolescents, falls and sports related trauma are often the causes of mTBI. Importantly, critical brain growth and development occurs during this sensitive period making the prospect of a brain injury a worrying phenomenon. Upwards of 70% of patients report circadian disruption following these injuries and this has been shown to impede recovery. Therefore, we sought to determine if core circadian clock gene expression was disrupted in rat model of repetitive mTBI (RmTBI). Male and female adolescent rats (n = 129) received sham or RmTBI. The animals were then euthanized at different times throughout the day and night. Tissue from the hypothalamus, cerebellum, hippocampus, liver, and small intestine were evaluated for the expression of per1, per2, cry1, clock, bmal1 and rev-erb-α. We found most clock genes varied across the day/night indicating circadian expression patterns. In the hypothalamus we found RmTBI altered the expression of cry1 and bmal1 in addition to sex differences in per2, cry1, clock, bmal1 and rev-erb- α. In the cerebellum, per1, per2, cry1, clock, bmal1 and rev-erb-α rhythms were all knocked out by RmTBI in addition to sex differences in cry1, clock and bmal1 expression. We also detected a significant decrease in overall expression of all clock genes in males in the middle of the night. In the hippocampus we found that RmTBI changed the rhythm of rev-erb-α expression in addition to sex differences in bmal1 expression. In the liver we detected strong rhythms in all genes examined, however only per2 expression was knocked out by RmTBI, in addition we also detected sex differences in per2 and cry1. We also detected an overall decrease in female clock gene expression in the early night. In the small intestine, RmTBI altered cry1 expression and there were sex differences in rev-erb-α. These results indicate that RmTBI alters core circadian clock gene expression in the central and peripheral nervous system in a time, tissue and sex dependent manner. This may be disrupting important phase relationships between the brain and peripheral nervous system and contributing to post-injury symptomology and also highlights the importance for time and sex dependent assessment of injury outcomes.

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来源期刊
Neurobiology of Sleep and Circadian Rhythms
Neurobiology of Sleep and Circadian Rhythms Neuroscience-Behavioral Neuroscience
CiteScore
4.50
自引率
0.00%
发文量
9
审稿时长
69 days
期刊介绍: Neurobiology of Sleep and Circadian Rhythms is a multidisciplinary journal for the publication of original research and review articles on basic and translational research into sleep and circadian rhythms. The journal focuses on topics covering the mechanisms of sleep/wake and circadian regulation from molecular to systems level, and on the functional consequences of sleep and circadian disruption. A key aim of the journal is the translation of basic research findings to understand and treat sleep and circadian disorders. Topics include, but are not limited to: Basic and translational research, Molecular mechanisms, Genetics and epigenetics, Inflammation and immunology, Memory and learning, Neurological and neurodegenerative diseases, Neuropsychopharmacology and neuroendocrinology, Behavioral sleep and circadian disorders, Shiftwork, Social jetlag.
期刊最新文献
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