Olivadoti M D, Opp M R
Neuroscience Graduate Program, University of Michigan, Ann Arbor, MI, USA.
Neuroscience. 2008 Apr 22;153(1):338-48. doi: 10.1016/j.neuroscience.2008.02.008. Epub 2008 Feb 19.
Cytokines in brain contribute to the regulation of physiological processes and complex behavior, including sleep. The cytokines that have been most extensively studied with respect to sleep are interleukin (IL)-1beta, tumor necrosis factor (TNF)-alpha, and IL-6. Administration of these cytokines into laboratory animals, or in some cases into healthy human volunteers, increases the amount of time spent in non-rapid eye movement (NREM) sleep. Although antagonizing the IL-1 or TNF systems reduces the amount of time laboratory animals spend in NREM sleep, interactions among these three cytokine systems as they pertain to the regulation of physiological NREM sleep are not well understood. To further elucidate mechanisms in brain by which IL-1beta, TNFalpha, and/or IL-6 contribute to NREM sleep regulation, we injected recombinant murine interleukin-1beta (muIL-1beta) into C57BL/6J mice and into IL-6-deficient mice (IL-6 knockout, KO). IL-6 KO (B6.129S6-Il6(tm1Kopf); n=13) and C57BL/6J mice (n=14) were implanted with telemeters to record the electroencephalogram (EEG) and core body temperature, as well as with indwelling guide cannulae targeted to one of the lateral ventricles. After recovery and habituation, mice were injected intracerebroventricularly just prior to dark onset on different days with either 0.5 microl vehicle (pyrogen-free saline; PFS) or with 0.5 microl PFS containing one of four doses of muIL-1beta (2.5 ng, 5 ng, 10 ng, 50 ng). No mouse received more than two doses of muIL-1beta, and administration of muIL-1beta doses was counter-balanced to eliminate potential order effects. Sleep-wake behavior was determined for 24 h after injections. i.c.v. administration of muIL-1beta increased in NREM sleep of both mouse strains in a dose-related fashion, but the maximal increase was of greater magnitude in C57Bl/6J mice. muIL-1beta induced fever in C57Bl/6J mice but not in IL-6 KO mice. Collectively, these data demonstrate IL-6 is necessary for IL-1 to induce fever, but IL-6 is not necessary for IL-1 to alter NREM sleep.
大脑中的细胞因子有助于调节生理过程和复杂行为,包括睡眠。在睡眠方面研究最为广泛的细胞因子是白细胞介素(IL)-1β、肿瘤坏死因子(TNF)-α和IL-6。将这些细胞因子注射到实验动物体内,或在某些情况下注射到健康人类志愿者体内,会增加非快速眼动(NREM)睡眠的时长。尽管拮抗IL-1或TNF系统会减少实验动物在NREM睡眠中的时长,但这三种细胞因子系统在生理NREM睡眠调节方面的相互作用尚不清楚。为了进一步阐明IL-1β、TNFα和/或IL-6在大脑中调节NREM睡眠的机制,我们将重组小鼠白细胞介素-1β(muIL-1β)注射到C57BL/6J小鼠和IL-6基因缺陷小鼠(IL-6基因敲除,KO)体内。将IL-6基因敲除小鼠(B6.129S6-Il6(tm1Kopf);n = 13)和C57BL/6J小鼠(n = 14)植入遥测器以记录脑电图(EEG)和核心体温,并植入靶向侧脑室之一的留置引导套管。恢复和适应后,在不同日期的黑暗开始前,给小鼠脑室内注射0.5微升载体(无热原生理盐水;PFS)或含有四种剂量muIL-1β(2.5纳克、5纳克、10纳克、50纳克)之一的0.5微升PFS。没有小鼠接受超过两剂muIL-1β,并且muIL-1β剂量的给药进行了平衡以消除潜在的顺序效应。注射后24小时测定睡眠-觉醒行为。脑室内注射muIL-1β以剂量相关的方式增加了两种小鼠品系的NREM睡眠,但C57Bl/6J小鼠的最大增加幅度更大。muIL-1β在C57Bl/6J小鼠中诱导发热,但在IL-6基因敲除小鼠中未诱导发热。总体而言,这些数据表明IL-6是IL-1诱导发热所必需的,但IL-6不是IL-1改变NREM睡眠所必需的。
