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两种品系小鼠的昼夜节律系统对GABA活性药物的不同反应。

Different responses of the circadian system to GABA-active drugs in two strains of mice.

作者信息

Ebihara S, Goto M, Oshima I

机构信息

Department of Animal Physiology, Faculty of Agriculture, Nagoya University, Japan.

出版信息

J Biol Rhythms. 1988 Winter;3(4):357-64. doi: 10.1177/074873048800300405.

Abstract

Recent work in our laboratory has shown that sodium pentobarbital injections can induce phase-dependent phase shifts of the circadian rhythm of locomotor activity with the maximum advance at circadian time (CT) 8 and the maximum delay at CT0 in SK/Nga mice but no phase shifts in C57BL/6 mice. In the present study, the possibility that the differences in the effects of pentobarbital on the circadian rhythm may be due to different contributions of the GABA-ergic system to circadian organization in the two strains was tested by comparing the responses of SK mice with those of C57BL mice to muscimol (2 mg/kg), a GABA receptor agonist, and triazolam (25 mg/kg), which is thought to act by potentiating the action of GABA. The hypothesis that pentobarbital-induced phase shifts of SK mice are mediated by the GABA receptor system was also tested by observing whether the phase-shifting effects of pentobarbital were blocked by bicuculline (0.5 mg/kg), a selective antagonist of GABA, injected 3 min prior to pentobarbital (30 mg/kg). The results indicated that muscimol induced phase advances at CT8 and phase delays at CT0, and triazolam induced phase advances at CT8 in SK mice. No phase shifts were induced by any treatment in C57BL mice. These results suggest that the role of GABA-ergic systems in circadian organization may be different in SK and C57BL mice. In addition, bicuculline could block the phase-shifting effects of pentobarbital in SK mice, suggesting that the GABA receptor system may mediate phase-shifting effects of pentobarbital in SK mice.

摘要

我们实验室最近的研究表明,戊巴比妥钠注射可诱导SK/Nga小鼠运动活动昼夜节律的相位依赖性相位偏移,在昼夜时间(CT)8时提前最大,在CT0时延迟最大,而C57BL/6小鼠则无相位偏移。在本研究中,通过比较SK小鼠和C57BL小鼠对GABA受体激动剂蝇蕈醇(2mg/kg)和据认为通过增强GABA作用而起作用的三唑仑(25mg/kg)的反应,测试了戊巴比妥对昼夜节律影响的差异可能是由于两种品系中GABA能系统对昼夜节律组织的不同贡献这一可能性。还通过观察戊巴比妥(30mg/kg)注射前3分钟注射的GABA选择性拮抗剂荷包牡丹碱(0.5mg/kg)是否能阻断戊巴比妥的相位偏移效应,来测试戊巴比妥诱导SK小鼠相位偏移由GABA受体系统介导这一假设。结果表明,蝇蕈醇在SK小鼠中诱导CT8时的相位提前和CT0时的相位延迟,三唑仑在SK小鼠中诱导CT8时的相位提前。C57BL小鼠的任何处理均未诱导相位偏移。这些结果表明,GABA能系统在昼夜节律组织中的作用在SK和C57BL小鼠中可能不同。此外,荷包牡丹碱可阻断戊巴比妥在SK小鼠中的相位偏移效应,表明GABA受体系统可能介导戊巴比妥在SK小鼠中的相位偏移效应。

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