在生长抑素阳性中间神经元中选择性消融3型腺苷酸环化酶会使小鼠出现焦虑和抑郁样行为。
Selective ablation of type 3 adenylyl cyclase in somatostatin-positive interneurons produces anxiety- and depression-like behaviors in mice.
作者信息
Yang Xiao-Yu, Ma Zhao-Liang, Storm Daniel R, Cao Hong, Zhang Yu-Qiu
机构信息
Department of Translational Neuroscience, Jing'an District Centre Hospital of Shanghai, State Key Laboratory of Medical Neurobiology and MOE Frontiers Center for Brain Science, Institutes of Brain Science, Institutes of Integrative Medicine, Fudan University, Shanghai 200032, China.
Department of Pharmacology, University of Washington, Seattle, WA 98105, United States.
出版信息
World J Psychiatry. 2021 Feb 19;11(2):35-49. doi: 10.5498/wjp.v11.i2.35.
BACKGROUND
Major depressive disorder (MDD) is a highly disabling psychiatric syndrome associated with deficits of specific subpopulations of cortical GABAergic interneurons; however, the underlying molecular mechanism remains unknown. Type 3 adenylyl cyclase (ADCY3, AC3), which is important for neuronal excitability, has been implicated in MDD in a genome-wide association study in humans. Moreover, a study reported that ablation of AC3 in mice caused similar symptoms as MDD patients.
AIM
To determine if disruption of the AC3 gene in different subtypes of GABAergic interneurons of mice causes depression-like behaviors.
METHODS
Using immunohistochemistry, we investigated the expression of AC3 in two major subtypes GABAergic interneurons: Somatostatin-positive (SST) and parvalbumin-positive (PV) neurons. Genetic manipulations were used to selectively disrupt AC3 expression in SST or PV interneurons. A series of behavior tests including rotarod test, open field test (OFT), elevated plus maze test (EPM), forced swimming test (FST), and tail suspension test (TST) were used to evaluate the motor ability, anxiety- and depression- like behaviors, respectively.
RESULTS
Our results indicate that approximately 90.41% of SST and 91.22% of PV interneurons express AC3. After ablation of AC3 in SST interneurons, the mice spent comparable time in the center area in OFT, but significantly less time in the open arms and low frequency of entries to the open arms in EPM. Furthermore, these mice showed prolonged immobility in FST and more freezing in TST. However, there were no significant changes in these behaviors after specific disruption of AC3 in PV interneurons.
CONCLUSION
This study indicates that ablation of AC3 in SST interneurons of mice increases anxiety- and depression-like behaviors in mice, supporting the general hypothesis that decreased AC3 activity may play a role in human depression.
背景
重度抑郁症(MDD)是一种严重致残的精神综合征,与皮质γ-氨基丁酸(GABA)能中间神经元的特定亚群缺陷有关;然而,其潜在的分子机制仍然未知。3型腺苷酸环化酶(ADCY3,AC3)对神经元兴奋性很重要,在一项人类全基因组关联研究中已表明其与MDD有关。此外,一项研究报告称,小鼠体内AC3的缺失会导致与MDD患者相似的症状。
目的
确定小鼠GABA能中间神经元不同亚型中AC3基因的破坏是否会导致抑郁样行为。
方法
我们使用免疫组织化学方法研究了AC3在两种主要亚型GABA能中间神经元中的表达:生长抑素阳性(SST)和小白蛋白阳性(PV)神经元。采用基因操作选择性破坏SST或PV中间神经元中AC3的表达。一系列行为测试,包括转棒试验、旷场试验(OFT)、高架十字迷宫试验(EPM)、强迫游泳试验(FST)和悬尾试验(TST),分别用于评估运动能力、焦虑样和抑郁样行为。
结果
我们的结果表明,约90.41%的SST中间神经元和91.22%的PV中间神经元表达AC3。在SST中间神经元中敲除AC3后,小鼠在OFT的中央区域停留时间相当,但在EPM的开放臂中停留时间显著减少,进入开放臂的频率较低。此外,这些小鼠在FST中表现出更长的不动时间,在TST中表现出更多的僵住。然而,在PV中间神经元中特异性破坏AC3后,这些行为没有显著变化。
结论
本研究表明,小鼠SST中间神经元中AC3的缺失会增加小鼠的焦虑样和抑郁样行为,支持AC3活性降低可能在人类抑郁症中起作用的一般假设。
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