Orexin A Decreases Ketamine-induced Anesthesia Time in the Rat: the Relevance to Brain Noradrenergic Neuronal Activity

Overview

Journal Anesth Analg

Specialty Anesthesiology

Date 2009 Jan 20

PMID 19151277

Citations 18

Authors

Ryuji Tose

Tetsuya Kushikata

Hitoshi Yoshida

Mihoko Kudo

Kenichi Furukawa

Shinya Ueno

Kazuyoshi Hirota

Affiliations

Soon will be listed here.

Abstract

Background: Orexins (OXs) regulate wakefulness, and a lack of OX Type-I receptors cause narcolepsy. OX selectively increases norepinephrine (NE) release from rat cerebral cortical slices, and brain noradrenergic neurons are involved in the sleep-wakefulness cycle. Ketamine increases NE release from the rat cerebral cortex. We hypothesized that OX would affect ketamine anesthesia's interactions with brain noradrenergic neuronal activity.

Methods: We used Sprague Dawley rats. We studied 1) in vivo effects of orexin A (OXA) and SB-334867-A (Orexin-1 receptor antagonist) on ketamine-induced anesthesia time, 2) in vivo effects of OXA on ketamine-induced increase in NE release from the frontal cortex assessed using microdialysis, and 3) in vitro effects of ketamine on OXA-evoked NE release from rat cerebrocortical slices.

Results: 1) Intracerebroventricular OXA 1 nmol significantly decreased ketamine anesthesia time by 20%-30% at 50, 100, and 125 mg/kg intraperitoneal (IP) ketamine. SB-334867-A fully reversed the decrease produced by OXA. 2) OXA also decreased the release of NE induced by ketamine even though OXA increased the release of NE in rat prefrontal cortex. Maximum NE release in Group OX + K (intracerebroventricular OXA 1 nmol + IP ketamine 100 mg/kg) was 271% and was significantly smaller than that in Group K (ketamine 100 mg/kg IP, 390% of baseline, P = 0.029). 3) Ketamine inhibited OX-evoked NE release with clinically relevant IC(50) values.

Conclusion: Orexinergic neurons may be an important target for ketamine. OXA antagonized ketamine anesthesia via Orexin-1 receptor with noradrenergic neurons.

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

Kushikata T, Hirota K, Saito J, Takekawa D Pharmaceuticals (Basel). 2021; 14(5).

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