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增强的紧张性抑制作用影响静脉麻醉药依托咪酯和丙泊酚的催眠和遗忘作用。

Enhanced tonic inhibition influences the hypnotic and amnestic actions of the intravenous anesthetics etomidate and propofol.

机构信息

Department of Neuroscience, Tufts University School of Medicine, Boston, Massachusetts 02111, USA.

出版信息

J Neurosci. 2013 Apr 24;33(17):7264-73. doi: 10.1523/JNEUROSCI.5475-12.2013.

DOI:10.1523/JNEUROSCI.5475-12.2013
PMID:23616535
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3685479/
Abstract

Intravenous anesthetics exert a component of their actions via potentiating inhibitory neurotransmission mediated by γ-aminobutyric type-A receptors (GABAARs). Phasic and tonic inhibition is mediated by distinct populations of GABAARs, with the majority of phasic inhibition by subtypes composed of α1-3βγ2 subunits, whereas tonic inhibition is dependent on subtypes assembled from α4-6βδ subunits. To explore the contribution that these distinct forms of inhibition play in mediating intravenous anesthesia, we have used mice in which tyrosine residues 365/7 within the γ2 subunit are mutated to phenyalanines (Y365/7F). Here we demonstrate that this mutation leads to increased accumulation of the α4 subunit containing GABAARs in the thalamus and dentate gyrus of female Y365/7F but not male Y365/7F mice. Y365/7F mice exhibited a gender-specific enhancement of tonic inhibition in the dentate gyrus that was more sensitive to modulation by the anesthetic etomidate, together with a deficit in long-term potentiation. Consistent with this, female Y365/7F, but not male Y365/7F, mice exhibited a dramatic increase in the duration of etomidate- and propofol-mediated hypnosis. Moreover, the amnestic actions of etomidate were selectively potentiated in female Y365/7F mice. Collectively, these observations suggest that potentiation of tonic inhibition mediated by α4 subunit containing GABAARs contributes to the hypnotic and amnestic actions of the intravenous anesthetics, etomidate and propofol.

摘要

静脉麻醉通过增强 γ-氨基丁酸 A 型受体 (GABAAR) 介导的抑制性神经传递发挥其作用的一部分。相移和紧张性抑制由不同群体的 GABAAR 介导,大多数相移抑制由由 α1-3βγ2 亚基组成的亚型介导,而紧张性抑制依赖于由 α4-6βδ 亚基组装的亚型。为了探讨这些不同形式的抑制在介导静脉麻醉中的作用,我们使用了酪氨酸残基 365/7 在 γ2 亚基中突变为苯丙氨酸 (Y365/7F) 的小鼠。在这里,我们证明这种突变导致雌性 Y365/7F 但不是雄性 Y365/7F 小鼠的丘脑和齿状回中含有 α4 亚基的 GABAAR 积累增加。Y365/7F 小鼠表现出性别特异性的紧张性抑制增强,对麻醉药依托咪酯的调节更为敏感,同时长时程增强受损。与此一致的是,只有雌性 Y365/7F 而不是雄性 Y365/7F 小鼠表现出依托咪酯和异丙酚介导的催眠作用的持续时间显著增加。此外,依托咪酯的健忘作用在雌性 Y365/7F 小鼠中被选择性增强。总的来说,这些观察结果表明,由含有 α4 亚基的 GABAAR 介导的紧张性抑制的增强有助于静脉麻醉药依托咪酯和异丙酚的催眠和健忘作用。

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