首页> 外文期刊>Behavioural Brain Research: An International Journal >Quinolinic acid lesions of the pedunculopontine nucleus impair sleep architecture, but not locomotion, exploration, emotionality or working memory in the rat.
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Quinolinic acid lesions of the pedunculopontine nucleus impair sleep architecture, but not locomotion, exploration, emotionality or working memory in the rat.

机译:人脚猿核的喹啉酸损害会损害睡眠结构,但不会损害大鼠的运动,探索,情绪或工作记忆。

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摘要

Anatomical and functional studies have shown that the NADPH-diaphorase-positive cholinergic neurons of the pedunculopontine nucleus (PPN) send projections to several areas in the brain. The purpose of this work was to investigate whether bilateral lesions with quinolinic acid, a neurotoxin with greater selectivity for NADPH-diaphorase-positive neurons, aimed at the compact portion of the PPN would affect the performance of adaptive behaviors, such as sleep, locomotion, and spontaneous alternation. Lesioned animals were divided in a low lesion group (LL, <50% neuron loss) and a high lesion group (HL, >/=50% neuron loss). The LL animals did not show any significant changes in sleep patterns, as compared to controls. In contrast, the HL group showed a significant increase in the number of REM sleep periods, and a reduction of REM sleep average duration, but did not differ in the total time spent in REM sleep. HL animals also showed an increase in the number of SWS periods, though wakefulness parameters did not show significant alterations. The duration and number of both REM and SWS sleep episodes were significantly correlated with the number of NADPH-diaphorase-positive neurons in the PPN. The short-term habituation pattern of locomotion, the vertical exploratory activity, as well as the thigmotaxis (an index of emotionality), displayed by LL and HL rats in a novel environment were similar to those of control animals. Likewise, there were no significant differences in spontaneous alternation among the groups. Our results indicate that quinolinic acid lesions of NADPH-diaphorase-positive cholinergic neurons localized in the posterior region of the PPN disrupt normal sleep structure, while motor activity and spontaneous alternation remain unaffected.
机译:解剖学和功能研究表明,小足猿核(PPN)的NADPH-心肌黄素酶阳性胆碱能神经元向大脑的多个区域发送投影。这项工作的目的是调查针对PPN紧凑部分的,对NADPH-心肌黄递酶阳性神经元具有更高选择性的神经毒素喹啉酸对双侧病变是否会影响适应行为的表现,例如睡眠,运动,和自发的交替。病变动物分为低病变组(LL,<50%神经元丢失)和高病变组(HL,> / = 50%神经元丢失)。与对照组相比,LL动物的睡眠方式没有任何显着变化。相反,HL组显示REM睡眠期数显着增加,REM睡眠平均持续时间减少,但在REM睡眠上花费的总时间没有差异。 HL动物的SWS周期数也有所增加,尽管清醒参数并未显示出明显的变化。 REM和SWS睡眠发作的持续时间和数目与PPN中NADPH-心肌黄递酶阳性神经元的数目显着相关。 LL和HL大鼠在新环境中表现出的短期运动习惯,垂直探索活动以及触觉行为(情绪指数)与对照动物相似。同样,各组之间的自发交替也无显着差异。我们的结果表明,位于PPN后部的NADPH-心肌黄素酶阳性胆碱能神经元的喹啉酸损伤会破坏正常的睡眠结构,而运动活动和自发性交替仍然不受影响。

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