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Sleep disruption elevates oxidative stress in parvalbumin-positive cells of the rat cerebral cortex

机译:睡眠破坏升高了大鼠脑皮层的Parvalbumin阳性细胞中的氧化应激

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We used a novel automated sleep disruption (SD) apparatus to determine the impact of SD on sleep and molecular markers of oxidative stress in parvalbumin (PV) neurons in the rat prefrontal cortex (PFC). Rats were subjected to two 6 hr SD sessions from zeitgeber time (ZT) 0 to ZT6, one by the gentle handling method and the other by an automated agitator running the length of the rat's home cage floor (a novel SD method). The same rats were later subjected to a 12 hr SD session from ZT0 to ZT12. Sleep was disrupted with both methods, although rats slept less during gentle handling than during the automated condition. Immediately after both SD sessions, rats displayed compensatory sleep characterized by elevated slow-wave activity. We measured in the prelimbic prefrontal cortex (prelimbic PFC; 6 and 12 hr SD) and orbital frontal cortex (12 hr SD) the intensity of the oxidative stress marker, 8-oxo-2′-deoxyguanosine (8-oxo-dG) as well as the staining intensity of PV and the PV cell-associated perineuronal net marker, Wisteria floribunda agglutinin (WFA). In the prelimbic PFC, 6 hr SD increased the intensity of 8-oxo-dG, PV, and WFA. After 12 hr SD, the intensity of 8-oxo-dG was elevated in all neurons. PV intensity was elevated only in neurons colabeled with 8-oxo-dG or WFA, and no changes were found in WFA intensity. We conclude that in association with SD-induced sleep drive, PV neurons in the prelimbic PFC exhibit oxidative stress. ? 2018 Sleep Research Society.
机译:我们使用了一种新颖的自动睡眠中断(SD)装置,以确定SD对大鼠前额叶皮质(PFC)中胰岛蛋白(PV)神经元氧化应激的睡眠和分子标记的影响。通过温和的处理方法,通过温和的搅拌器进行两次从Zeitgeber时间(ZT)0至ZT6的大鼠从Zeitgeber时间(ZT)0到ZT6进行两次,通过自动搅拌器运行大鼠家庭笼式地板的长度(新颖的SD方法)。后面将与ZT0至ZT12的12小时SD会议进行相同的大鼠。两种方法都扰乱了睡眠,尽管在温和的处理过程中的大鼠比在自动化条件下睡得更少。在两个SD会话后立即显示,大鼠显示了慢波活动升高的补偿性睡眠。我们在预先预称皮质(PRELIMBIC PFC; 6和12 HR SD)和轨道正面皮质(12小时SD)中测量的氧化应激标记物的强度,8-氧代-2'-脱氧核苷酸(8-氧代-DG)为以及PV的染色强度和PV细胞相关的羽毛尿净标题,Wisteria Floribunda algGlutinin(WFA)。在PRELIMBIC PFC中,6小时SD增加了8-氧代-DG,PV和WFA的强度。在12小时后,在所有神经元中升高了8-氧代-DG的强度。 PV强度仅在用8-氧代-DG或WFA共英中标记的神经元升高,并且在WFA强度中没有发现变化。我们得出结论,与SD诱导的睡眠驱动相关联,PVIMBIC PFC中的PV神经元表现出氧化应激。还2018年睡眠研究会。

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