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视交叉上核中 GABA 的兴奋性效应的功能意义。

Functional Significance of the Excitatory Effects of GABA in the Suprachiasmatic Nucleus.

机构信息

Neuroscience Institute and Center for Behavioral Neuroscience, Georgia State University, Atlanta, GA, USA.

出版信息

J Biol Rhythms. 2018 Aug;33(4):376-387. doi: 10.1177/0748730418782820. Epub 2018 Jul 5.

Abstract

Over 90% of neurons within the suprachiasmatic nucleus (SCN) express γ-aminobutyric acid (GABA). Although GABA is primarily an inhibitory neurotransmitter, in vitro studies suggest that the activation of GABA receptors (GABAR) elicits excitation in the adult SCN. The ratio of excitatory to inhibitory responses to GABA depends on the balance of chloride influx by Na-K-Cl cotransporter 1 (NKCC1) and chloride efflux by K-Cl cotransporters (KCCs). Excitatory responses to GABA can be blocked by inhibition of the inward chloride cotransporter, NKCC1, with the loop diuretic bumetanide. Here we investigated the role of NKCC1 activity in phase shifting the circadian pacemaker in response to photic and nonphotic signals in male Syrian hamsters housed in constant darkness. In the early subjective night (CT 13.5), injection of bumetanide into the SCN reduced light-induced phase delays. However, during the late subjective night (CT 19), bumetanide administration did not alter light-induced phase advances. Injection of bumetanide during the subjective day (CT 6) did not alter the phase of free-running circadian rhythms but attenuated phase advances induced by injection of the GABAR agonist muscimol into the SCN. These data support the hypothesis that the excitatory effects of endogenously released GABA contribute to the ability of light to induce phase delays, thereby contributing to the most important function of the circadian system, its entrainment with the day-night cycle. Further, the finding that bumetanide inhibits the phase-advancing effects of muscimol during the subjective day supports the hypothesis that the excitatory responses to GABA also contribute to the ability of nonphotic stimuli to phase shift the circadian pacemaker.

摘要

超过 90%的视交叉上核(SCN)神经元表达γ-氨基丁酸(GABA)。虽然 GABA 主要是一种抑制性神经递质,但体外研究表明,GABA 受体(GABAR)的激活会在成年 SCN 中引起兴奋。GABA 对兴奋性和抑制性反应的比率取决于 Na-K-Cl 共转运蛋白 1(NKCC1)氯离子内流和 K-Cl 共转运蛋白(KCCs)氯离子外排之间的平衡。通过抑制内向氯离子共转运蛋白 NKCC1,用Loop 利尿剂布美他尼(bumetanide)可以阻断 GABA 的兴奋性反应。在这里,我们研究了 NKCC1 活性在对光和非光信号响应中对生物钟起搏相位的作用,研究对象是处于持续黑暗环境中的雄性叙利亚仓鼠。在早期主观夜间(CT 13.5),将布美他尼注入 SCN 会减少光诱导的相位延迟。然而,在晚期主观夜间(CT 19),布美他尼给药不会改变光诱导的相位提前。在主观白天(CT 6)期间注射布美他尼不会改变自由运行的昼夜节律的相位,但会减弱 SCN 中 GABA 受体激动剂 muscimol 注射引起的相位提前。这些数据支持了这样的假设,即内源性释放的 GABA 的兴奋性作用有助于光诱导相位延迟的能力,从而有助于生物钟系统的最重要功能,即与昼夜节律的同步。此外,发现布美他尼在主观白天抑制 muscimol 的相位提前作用支持了这样的假设,即 GABA 的兴奋性反应也有助于非光刺激使生物钟起搏相位移动的能力。

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