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在大鼠脑桥微量注射卡巴胆碱并不能可靠地增强异相睡眠。

Pontine microinjection of carbachol does not reliably enhance paradoxical sleep in rats.

作者信息

Deurveilher S, Hars B, Hennevin E

机构信息

Laboratoire de Neurobiologie de l'Apprentissage et de la Mémoire, Université Paris-Sud, Orsay, France.

出版信息

Sleep. 1997 Aug;20(8):593-607.

PMID:9351126
Abstract

It has been repeatedly shown in cats that acute administration of carbachol into the pontine reticular formation (PRF) readily evokes a state that closely mimics natural paradoxical sleep (PS). Surprisingly, there are few corresponding studies in rats. In order to further characterize the effects of pontine carbachol in rats, 151 injections of different doses (from 3 micrograms to 0.005 microgram in 0.1 microliter saline) of carbachol were made at different sites within the PRF of 70 rats. Sleep-waking states obtained in the 4 hours following carbachol administration were compared to control values, obtained both under baseline condition (no injection) and following pontine injection of 0.1 microliter saline. On the one hand, from the whole set of carbachol injections, it appeared that: 1) most injections (112/151) did not significantly alter the sleep-wake states; 2) when carbachol was effective, it induced either increased PS (20 injections) or increased waking (19 injections); and 3) effective injection sites were intermingled with noneffective sites. Dose- or site-dependency effects can account in part, but not totally, for these discordant results. On the other hand, in accordance with previous rat studies, we found that: 1) the PRF medial and ventral to the motor trigeminal nucleus was the most effective region for carbachol to increase PS; 2) carbachol-induced PS enhancement was of moderate magnitude (+60% above control saline level over the 4-hour recording time); 3) latency to onset of the first PS episode was not shortened; and 4) only the number of PS episodes was increased, their duration was not prolonged. These characteristics of carbachol-induced PS enhancement strongly differ, both in terms of magnitude and timing, from those described in cats. We suggest that the less reliable and weaker effects of pontine carbachol injection in rats compared to cats can be due to methodological problems inherent in the intracerebral microinjection technique and also to species-related differences in the mechanisms controlling the PS state.

摘要

在猫身上反复证明,向脑桥网状结构(PRF)急性注射卡巴胆碱很容易诱发一种与自然异相睡眠(PS)极为相似的状态。令人惊讶的是,在大鼠身上进行的相应研究很少。为了进一步描述脑桥卡巴胆碱对大鼠的影响,对70只大鼠的PRF内不同部位进行了151次不同剂量(0.1微升盐水中从3微克到0.005微克)的卡巴胆碱注射。将注射卡巴胆碱后4小时内获得的睡眠-觉醒状态与在基线条件下(未注射)和脑桥注射0.1微升盐水后获得的对照值进行比较。一方面,从整个卡巴胆碱注射组来看,似乎:1)大多数注射(112/151)并未显著改变睡眠-觉醒状态;2)当卡巴胆碱有效时,它要么诱导PS增加(20次注射),要么诱导觉醒增加(19次注射);3)有效注射部位与无效部位相互交织。剂量或部位依赖性效应可以部分但不能完全解释这些不一致的结果。另一方面,根据先前对大鼠的研究,我们发现:1)运动三叉神经核内侧和腹侧的PRF是卡巴胆碱增加PS最有效的区域;2)卡巴胆碱诱导的PS增强幅度适中(在4小时记录时间内比对照盐水水平高60%);3)首次PS发作的起始潜伏期未缩短;4)仅PS发作次数增加,其持续时间未延长。卡巴胆碱诱导的PS增强的这些特征在幅度和时间方面与猫身上描述的特征有很大不同。我们认为,与猫相比,大鼠脑桥注射卡巴胆碱的效果不太可靠且较弱,可能是由于脑内微注射技术固有的方法学问题,也可能是由于控制PS状态的机制存在物种相关差异。

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