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Effect of two GABA-ergic drugs on the cognitive functions of rapid eye movement in sleep-deprived and recovered rats

机译:两种GABA刺激性药物对睡眠不足和恢复的大鼠快速眼动认知功能的影响

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摘要

Rapid eye movement (REM) sleep is closely associated with nervous functions. The present study aimed to evaluate the effects of gabazine and tiagabine on the cognitive functions (CF) of REM sleep-deprived and sleep recovered rats. Rats were divided into REM sleep deprivation, blank control (CC) and environmental groups. The REM sleep deprivation group was further divided into non-operation (nonOP), sham-operated (Sham), gabazine (SR) and tiagabine groups. Each group was evaluated over five time points: Sleep deprived for 1 day (SD 1 day), SD 3 day, SD 5 day, sleep recovery 6 h (RS 6 h) and RS 12 h. A rat model of REM sleep deprivation was established by a modified multi-platform water method, with CF assessed by Morris water maze. Hypothalamic γ-aminobutyric acid (GABA) and glutamic acid contents were measured via high performance liquid chromatography. The number and morphology of hypocretin (Hcrt) neurons and Fos in the hypothalamus, and GABAARα1-induced integral optical density were detected by immunofluorescence. Compared to the CC group, the nonOP and Sham group rats CF were significantly diminished, Fos-positive and Fos-Hcrt double positive cells were significantly increased, and GABA content and GABAARα1 expression levels were significantly elevated (P<0.05). The tiagabine and CC groups exhibited similar results at three time points. The CF of rats in the SR group were diminished and the number of Fos-positive and Fos-Hcrt double positive cells were significantly increased (P<0.05) at RS 6 h and RS l2 h. GABA content and GABAARα1 expression levels were significantly increased in the SR group at all time points (P<0.05), whereas only GABAARα1 expression levels were significantly increased in the tiagabine group at SD 5 day (P<0.05). The results of the present study indicated that REM sleep deprivation diminished CF, increased the number of Hcrt neurons, GABA content and GABAARα1 expression. Furthermore, all alterations were positively correlated with deprivation time and corrected by sleep recovery, as demonstrated by single-factor multi-level variance analysis at the various time points in each group. Therefore, the Hcrt nervous system may be an eligible therapeutic target for the treatment of insomnia.
机译:快速眼动(REM)睡眠与神经功能密切相关。本研究旨在评估加巴嗪和替加滨对REM睡眠剥夺和睡眠恢复大鼠的认知功能(CF)的影响。将大鼠分为REM睡眠剥夺,空白对照组(CC)和环境组。 REM睡眠剥夺组进一步分为非手术组(nonOP),假手术组(Sham),加巴嗪(SR)和替加滨组。在五个时间点对每个组进行评估:剥夺睡眠1天(SD 1天),SD 3天,SD 5天,睡眠恢复6 h(RS 6 h)和RS 12 h。通过改良的多平台水法建立了REM睡眠剥夺的大鼠模型,并通过Morris水迷宫评估了CF。通过高效液相色谱法测定下丘脑γ-氨基丁酸(GABA)和谷氨酸含量。通过免疫荧光检测下丘脑中降钙素(Hcrt)神经元和Fos的数量和形态,以及GABAARα1诱导的积分光密度。与CC组相比,nonOP组和Sham组大鼠的CF明显减少,Fos阳性和Fos-Hcrt双阳性细胞明显增加,GABA含量和GABAARα1表达水平显着升高(P <0.05)。替加滨和CC组在三个时间点上显示出相似的结果。 SR组大鼠的CF减少,在RS 6 h和RS 12 h时,Fos阳性和Fos-Hcrt双阳性细胞数量显着增加(P <0.05)。 SR组在所有时间点的GABA含量和GABAARα1表达水平均显着升高(P <0.05),而在tiagabine组中仅在SD 5天时GABA含量显着升高(P <0.05)。本研究的结果表明,REM睡眠剥夺减少了CF,增加了Hcrt神经元的数量,GABA含量和GABAARα1表达。此外,所有改变均与剥夺时间呈正相关,并通过睡眠恢复得到纠正,如每组各个时间点的单因素多级方差分析所表明的。因此,Hcrt神经系统可能是治疗失眠的合格治疗靶标。

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