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在异氟烷麻醉期间,食欲素通过大鼠基底前脑的食欲素-1受体增加皮质乙酰胆碱释放和脑电图激活。

Orexins increase cortical acetylcholine release and electroencephalographic activation through orexin-1 receptor in the rat basal forebrain during isoflurane anesthesia.

作者信息

Dong Hai-long, Fukuda Satoru, Murata Eri, Zhu Zhenghua, Higuchi Takashi

机构信息

Department of Anesthesiology & Reanimatology, Faculty of Medical Science, University of Fukui, Fukui, Japan..

出版信息

Anesthesiology. 2006 May;104(5):1023-32. doi: 10.1097/00000542-200605000-00019.

Abstract

BACKGROUND

Cholinergic arousal system plays an important role in the maintenance of consciousness. The authors investigated whether the intrabasalis injection of orexin-A or orexin-B and the electrically stimulated pedunculopontine tegmentum nuclei (PPTg: the origin of cholinergic ascending pathways) may alter acetylcholine efflux and electroencephalographic activity in the somatosensory cortex in relation to the orexinergic system in isoflurane-anesthetized rats.

METHODS

Either orexin-A (10, 30, or 100 pmol) or orexin-B (10, 30, or 100 pmol) (n = 6 each) was injected into the basal forebrain while the electroencephalogram was measured during 1.0 minimum alveolar concentration (1.2%) isoflurane anesthesia. Injection of Ringer's solution was used as a control. The PPTg was electrically stimulated twice with the following conditions: 1-s stimulus train (0.2 ms, 100 Hz, 400 microA) per min for 20 min. Twenty minutes before the second PPTg stimulation, Ringer's solution or 20 microg SB334867, an orexin-1 receptor antagonist (n = 5 each) was injected into the basal forebrain.

RESULTS

Injection of orexin-A (30 and 100 pmol) and orexin-B (100 pmol) significantly increased the acetylcholine efflux in the somatosensory cortex (P < 0.05). Injection of orexin-A (10, 30, 100 pmol) and orexin-B (30, 100 pmol) changed the burst and suppression patterns to arousal electroencephalogram. Compared with orexin-B, injection of a lower dose of orexin-A induced increase in the acetylcholine efflux and arousal electroencephalogram. SB334867 significantly attenuated the increases in the acetylcholine efflux and electroencephalographic activation evoked by PPTg stimulation.

CONCLUSION

The authors demonstrated that orexin-A was more potent than orexin-B in producing alteration of cholinergic basal forebrain neuronal activity and that the cortical activation induced by the PPTg stimulation against isoflurane anesthesia may be mediated through the orexin-1 receptors in the basal forebrain.

摘要

背景

胆碱能觉醒系统在意识维持中起重要作用。作者研究了在异氟烷麻醉的大鼠中,向基底前脑内注射食欲素-A或食欲素-B以及电刺激脚桥被盖核(PPTg:胆碱能上行通路的起源)是否会改变体感皮层中的乙酰胆碱外流和脑电图活动,这与食欲素能系统有关。

方法

在1.0最低肺泡浓度(1.2%)异氟烷麻醉期间测量脑电图时,将食欲素-A(10、30或100皮摩尔)或食欲素-B(10、30或100皮摩尔)(每组n = 6)注入基底前脑。注射林格氏液作为对照。对PPTg进行两次电刺激,条件如下:每分钟1次刺激串(0.2毫秒,100赫兹,400微安),持续20分钟。在第二次PPTg刺激前20分钟,将林格氏液或20微克SB334867(一种食欲素-1受体拮抗剂,每组n = 5)注入基底前脑。

结果

注射食欲素-A(30和100皮摩尔)和食欲素-B(100皮摩尔)显著增加了体感皮层中的乙酰胆碱外流(P < 0.05)。注射食欲素-A(10、30、100皮摩尔)和食欲素-B(30、100皮摩尔)将爆发和抑制模式转变为觉醒脑电图。与食欲素-B相比,注射较低剂量的食欲素-A可诱导乙酰胆碱外流增加和觉醒脑电图。SB334867显著减弱了PPTg刺激引起的乙酰胆碱外流增加和脑电图激活。

结论

作者证明,在产生胆碱能基底前脑神经元活动改变方面,食欲素-A比食欲素-B更有效,并且PPTg刺激对抗异氟烷麻醉诱导的皮层激活可能通过基底前脑的食欲素-1受体介导。

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