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Humoral Sleep Regulation; Interleukin-1 and Tumor Necrosis Factor

机译:体液睡眠调节;白细胞介素1与肿瘤坏死因子

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摘要

Two substances, the cytokines interleukin-1 beta (IL1β) and tumor necrosis factor alpha (TNFα), known for their many physiological roles, for example, cognition, synaptic plasticity, and immune function, are also well characterized in their actions of sleep regulation. These substances promote non-rapid eye movement sleep and can induce symptoms associated with sleep loss such as sleepiness, fatigue, and poor cognition. IL1β and TNFα are released from glia in response to extracellular ATP. They bind to their receptors on neurons resulting in neuromodulator and neurotransmitter receptor up/downregulation (e.g., adenosine and glutamate receptors) leading to altered neuronal excitability and function, that is, a state change in the local network. Synchronization of state between local networks leads to emergent whole brain oscillations, such as sleep/wake cycles.
机译:细胞因子白介素-1β(IL1β)和肿瘤坏死因子α(TNFα)这两种物质以其许多生理作用而著称,例如认知,突触可塑性和免疫功能,它们在睡眠调节作用中也具有很好的特征。 。这些物质可促进眼动运动,使人无法快速入睡,并可诱发与睡眠不足有关的症状,如嗜睡,疲劳和认知能力差。 IL1β和TNFα响应于细胞外ATP而从神经胶质中释放。它们与神经元上的受体结合,导致神经调节剂和神经递质受体的上调/下调(例如腺苷和谷氨酸受体),导致神经元兴奋性和功能改变,即局域网中的状态改变。局域网之间的状态同步会导致出现整个大脑振荡,例如睡眠/唤醒循环。

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