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食欲素神经元中的Fos表达随行为状态而变化。

Fos expression in orexin neurons varies with behavioral state.

作者信息

Estabrooke I V, McCarthy M T, Ko E, Chou T C, Chemelli R M, Yanagisawa M, Saper C B, Scammell T E

机构信息

Department of Neurology, Beth Israel Deaconess Medical Center, Boston, Massachusetts 02115, USA.

出版信息

J Neurosci. 2001 Mar 1;21(5):1656-62. doi: 10.1523/JNEUROSCI.21-05-01656.2001.

Abstract

The neuropeptide orexin (also known as hypocretin) is hypothesized to play a critical role in the regulation of sleep-wake behavior. Lack of orexin produces narcolepsy, which is characterized by poor maintenance of wakefulness and intrusions of rapid eye movement (REM) sleep or REM sleep-like phenomena into wakefulness. Orexin neurons heavily innervate many aminergic nuclei that promote wakefulness and inhibit REM sleep. We hypothesized that orexin neurons should be relatively active during wakefulness and inactive during sleep. To determine the pattern of activity of orexin neurons, we recorded sleep-wake behavior, body temperature, and locomotor activity under various conditions and used double-label immunohistochemistry to measure the expression of Fos in orexin neurons of the perifornical region. In rats maintained on a 12 hr light/dark cycle, more orexin neurons had Fos immunoreactive nuclei during the night period; in animals housed in constant darkness, this activation still occurred during the subjective night. Sleep deprivation or treatment with methamphetamine also increased Fos expression in orexin neurons. In each of these experiments, Fos expression in orexin neurons correlated positively with the amount of wakefulness and correlated negatively with the amounts of non-REM and REM sleep during the preceding 2 hr. In combination with previous work, these results suggest that activation of orexin neurons may contribute to the promotion or maintenance of wakefulness. Conversely, relative inactivity of orexin neurons may allow the expression of sleep.

摘要

神经肽食欲素(也称为下丘脑泌素)被认为在睡眠 - 觉醒行为的调节中起关键作用。缺乏食欲素会导致发作性睡病,其特征是觉醒难以维持,快速眼动(REM)睡眠或类似REM睡眠的现象侵入觉醒状态。食欲素神经元大量支配许多促进觉醒并抑制REM睡眠的胺能核团。我们推测食欲素神经元在觉醒期间应相对活跃,而在睡眠期间不活跃。为了确定食欲素神经元的活动模式,我们在各种条件下记录了睡眠 - 觉醒行为、体温和运动活动,并使用双标免疫组织化学法测量穹窿周区域食欲素神经元中Fos的表达。在维持12小时光照/黑暗周期的大鼠中,夜间有更多的食欲素神经元具有Fos免疫反应性细胞核;在持续黑暗环境饲养的动物中,这种激活仍发生在主观夜间。睡眠剥夺或用甲基苯丙胺治疗也会增加食欲素神经元中Fos的表达。在这些实验中的每一个中,食欲素神经元中Fos的表达与觉醒量呈正相关,与前2小时非REM睡眠和REM睡眠量呈负相关。结合先前的研究工作,这些结果表明食欲素神经元的激活可能有助于促进或维持觉醒。相反,食欲素神经元的相对不活跃可能允许睡眠的表现。

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