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睡眠剥夺期间基底前脑中外周血清素和多巴胺代谢物水平的增加。

Increases in extracellular serotonin and dopamine metabolite levels in the basal forebrain during sleep deprivation.

机构信息

Institute of Biomedicine, Physiology, University of Helsinki, Helsinki, Finland.

出版信息

Brain Res. 2011 Jul 5;1399:40-8. doi: 10.1016/j.brainres.2011.05.008. Epub 2011 May 14.

DOI:10.1016/j.brainres.2011.05.008
PMID:21645878
Abstract

The basal forebrain (BF) is an important mediator of cortical arousal, which is innervated by all ascending arousal systems. During sleep deprivation (SD) a site-specific accumulation of sleep factors in the BF results in increased sleep pressure (Kalinchuk et al., 2006; Porkka-Heiskanen et al., 1997; Porkka-Heiskanen et al., 2000). However, animals are able to stay awake and even increase their neuronal activity in the BF and cortex during SD, suggesting increased activity of the ascending arousal systems to counteract the effect of sleep pressure. This study used in vivo microdialysis to measure the effect of a 6h SD, by "gentle handling" in freely moving rats, on the extracellular levels of serotonin and dopamine metabolites (5-HIAA, and DOPAC and HVA respectively) in the BF. Additionally, because glucocorticoids can interact with monoaminergic neurotransmission, and SD could be stressful, corticosterone levels were measured. We found an increase in extracellular serotonin and dopamine metabolite levels (n=8, p≤0.05). No interaction between corticosterone and the monoaminergic systems was apparent. Extracellular corticosterone levels showed no increase during the first 3h of SD, and the subsequent increase (n=8, p≤0.05) did not result in values exceeding the normal diurnal maximum, indicating that no substantial stress was induced. The results demonstrate that SD increases extracellular dopamine and serotonin metabolites in the BF, suggesting increased activity of the ascending arousal systems. It remains to be investigated what the specific roles of the dopaminergic and serotonergic ascending arousal systems are in BF-mediated cortical arousal.

摘要

基底前脑(BF)是皮质觉醒的重要调节者,所有上行觉醒系统都支配着 BF。在睡眠剥夺(SD)期间,BF 中睡眠因子的特异性积累会导致睡眠压力增加(Kalinchuk 等人,2006 年;Porkka-Heiskanen 等人,1997 年;Porkka-Heiskanen 等人,2000 年)。然而,动物在 SD 期间能够保持清醒,甚至增加 BF 和皮质的神经元活动,这表明上行觉醒系统的活动增加以抵消睡眠压力的影响。本研究使用活体微透析技术测量了 6 小时 SD(通过自由移动大鼠的“轻柔处理”)对 BF 中 5-羟色胺和多巴胺代谢物(5-HIAA、DOPAC 和 HVA 分别)的细胞外水平的影响。此外,由于糖皮质激素可以与单胺能神经传递相互作用,SD 可能具有应激性,因此测量了皮质酮水平。我们发现细胞外 5-羟色胺和多巴胺代谢物水平增加(n=8,p≤0.05)。皮质酮和单胺能系统之间没有明显的相互作用。在 SD 的前 3 小时,细胞外皮质酮水平没有增加,随后的增加(n=8,p≤0.05)并没有导致值超过正常的昼夜最大值,表明没有引起实质性的应激。结果表明,SD 增加了 BF 中的细胞外多巴胺和 5-羟色胺代谢物,表明上行觉醒系统的活动增加。仍需研究 BF 介导的皮质觉醒中多巴胺能和 5-羟色胺能上行觉醒系统的具体作用。

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