Literature DB >> 28228241

Neuropeptide S reduces propofol- or ketamine-induced slow wave states through activation of cognate receptors in the rat.

Xiang-Pan Kong1, Can Wang2, Jun-Fan Xie2, Peng Zhao2, Li-Rong Dai2, Yu-Feng Shao3, Jian-Sheng Lin4, Yi-Ping Hou5.   

Abstract

Intracerebroventricular injection of NPS reduces the duration of the ketamine- or thiopental-induced loss of the righting reflex in rats. But the specific EEG activities are unknown. We therefore sought to examine the effects of the NPS-NPSR system on anesthetic-induced characteristics of EEG power spectra and sleep-wake profiles. NPS alone or together with an NPSR antagonist was injected intracerebroventricularly, whereas the propofol (50mg/kg) or ketamine (100mg/kg) was administrated intraperitoneally. NPS (1 or 2nmol) significantly reduced the amount of propofol-induced EEG delta activity and slow wave states (SWS). NPS (1 or 5nmol) significantly reduced the amount of ketamine-induced SWS and EEG delta activity. Cortical EEG power spectral analysis showed that, in saline-pretreated rats, propofol induced a marked increase in delta (0.5-4Hz) activity, decrease in theta (4.5-8.5Hz) activity, and decrease in high frequency activity (14.5-60Hz), while, in rats pretreated with 1nmol of NPS, the duration of delta activity was reduced, while its spectral pattern was not changed. Whereas injection of ketamine into saline-pretreated rats induced a marked increase in delta (0.5-4Hz) activity, a moderate increase in theta (4.5-8.5Hz) activity, and a marked decrease in high frequency (14.5-60Hz) activity. However, delta activity was reduced while theta activity increased under pretreatment with 1nmol of NPS. The inhibitory effect of NPS on anesthetic-induced SWS was characterized by a reduced SWS episode duration with no significant change in either episode number or latency to SWS. [D-Val5]NPS, an NPSR antagonist (20nmol), significantly attenuated the arousal-promoting effect of 1nmol of NPS, but had no effect on SWS when injected alone. We speculate that NPS significantly reduces anesthetic-induced SWS and EEG slow activity by selective activation of the NPSR, which, in turn, would trigger subsequent arousal pathways.
Copyright © 2017 Elsevier Ltd. All rights reserved.

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Year:  2017        PMID: 28228241     DOI: 10.1016/j.npep.2017.02.081

Source DB:  PubMed          Journal:  Neuropeptides        ISSN: 0143-4179            Impact factor:   3.286


  4 in total

1.  Central noradrenergic activity affects analgesic effect of Neuropeptide S.

Authors:  Kei Jinushi; Tetsuya Kushikata; Takashi Kudo; Girolamo Calo; Remo Guerrini; Kazuyoshi Hirota
Journal:  J Anesth       Date:  2017-11-11       Impact factor: 2.078

2.  Neuropeptide S Attenuates the Alarm Pheromone-Evoked Defensive and Risk Assessment Behaviors Through Activation of Cognate Receptor-Expressing Neurons in the Posterior Medial Amygdala.

Authors:  Yu-Feng Shao; Can Wang; Xiao-Ping Rao; Hua-Dong Wang; Yan-Li Ren; Jing Li; Chao-Yu Dong; Jun-Fan Xie; Xing-Wen Yang; Fu-Qiang Xu; Yi-Ping Hou
Journal:  Front Mol Neurosci       Date:  2021-12-24       Impact factor: 5.639

Review 3.  Roles of Neuropeptide S in Anesthesia, Analgesia, and Sleep.

Authors:  Tetsuya Kushikata; Kazuyoshi Hirota; Junichi Saito; Daiki Takekawa
Journal:  Pharmaceuticals (Basel)       Date:  2021-05-19

4.  Gene polymorphisms (rs324957, rs324981) in NPSR1 are associated with increased risk of primary insomnia: A cross-sectional study.

Authors:  Yuping Xie; Yuan Zhao; Liya Zhou; Lijun Zhao; Jinfeng Wang; Wei Ma; Xiaoyan Su; Peilin Hui; Bin Guo; Yu Liu; Jie Fan; Shangli Zhang; Jun Yang; Wenjuan Chen; Jing Wang
Journal:  Medicine (Baltimore)       Date:  2020-08-21       Impact factor: 1.817

  4 in total

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