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5,7-二氢麦角隐亭对仓鼠血清素能系统的破坏:对昼夜节律相位、同步化及对三唑仑反应的影响

Destruction of the hamster serotonergic system by 5,7-DHT: effects on circadian rhythm phase, entrainment and response to triazolam.

作者信息

Smale L, Michels K M, Moore R Y, Morin L P

机构信息

Department of Psychiatry, State University of New York, Stony Brook 11794-8101.

出版信息

Brain Res. 1990 May 7;515(1-2):9-19. doi: 10.1016/0006-8993(90)90570-2.

Abstract

The role of the serotonergic system in the regulation of hamster circadian rhythms was analyzed using intraventricular injection of the selective neurotoxin, 5,7-dihydroxytryptamine (5,7-DHT). Sixty days after 5,7-DHT administration, immunoreactive serotonin in the forebrain, particularly the suprachiasmatic nuclei and intergeniculate leaflets, was severely depleted in 16 animals, moderately depleted in four and only slightly affected in four. 5,7-DHT produced an immediate and sustained advance of the onset of running wheel activity relative to the 24 h light-dark (LD) cycle. Activity onset occurred 0.7 +/- 0.07 h before lights out among 5,7-DHT-treated animals compared with 0.18 +/- 0.04 h after lights out for vehicle-infused controls. This new, advanced phase angle of entrainment was maintained throughout the 60-day period of the study while the animals remained in a LD cycle, including after an 8-h phase advance of the light cycle. 5,7-DHT treatment also delayed the offset of wheelrunning in 16 of 24 animals and reduced the likelihood of a smooth pattern of reentrainment to the shifted LD cycle. The drug treatment did not affect circadian period in constant darkness, the rate of reentrainment to an 8-h phase advance or the amount of wheelrunning activity per day. In addition, 5,7-DHT treatment had no effect on the ability of triazolam, a short-acting benzodiazepine, to accelerate the rate of reentrainment to an 8-h phase advance. These observations show that ascending projections of midbrain raphe serotonin neurons participate in the regulation of the circadian activity phase but are not required for triazolam-induced acceleration of reentrainment to a phase-advanced LD cycle.

摘要

使用脑室内注射选择性神经毒素5,7 - 二羟基色胺(5,7 - DHT)分析了血清素能系统在调节仓鼠昼夜节律中的作用。给予5,7 - DHT 60天后,24只动物中,16只前脑,特别是视交叉上核和间膝叶中的免疫反应性血清素严重耗竭,4只中度耗竭,4只仅受到轻微影响。相对于24小时明暗(LD)循环,5,7 - DHT使跑步轮活动的开始时间立即且持续提前。与注射溶剂的对照组在熄灯后0.18±0.04小时开始活动相比,5,7 - DHT处理的动物在熄灯前0.7±0.07小时开始活动。在整个60天的研究期间,当动物处于LD循环时,包括在光周期提前8小时后,这种新的、提前的夹带相位角得以维持。5,7 - DHT处理还使24只动物中的16只跑步轮活动的结束时间延迟,并降低了重新适应转移后的LD循环的平滑模式的可能性。药物处理在持续黑暗中不影响昼夜节律周期、重新适应提前8小时相位的速率或每天的跑步轮活动量。此外,5,7 - DHT处理对短效苯二氮䓬类药物三唑仑加速重新适应提前8小时相位的速率的能力没有影响。这些观察结果表明,中脑缝际血清素神经元的上行投射参与昼夜活动相位的调节,但不是三唑仑诱导的加速重新适应提前相位的LD循环所必需的。

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