Ablation of Type III Adenylyl Cyclase in Mice Causes Reduced Neuronal Activity, Altered Sleep Pattern, and Depression-like Phenotypes

Abstract Background Although major depressive disorder (MDD) has low heritability, a genome-wide association study in humans has recently implicated type 3 adenylyl cyclase (AC3; ADCY3 ) in MDD. Moreover, the expression level of AC3 in blood has been considered as a MDD biomarker in humans. Neverthe...

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Published in:Biological psychiatry (1969) 2016-12, Vol.80 (11), p.836-848
Main Authors: Chen, Xuanmao, Luo, Jie, Leng, Yihua, Yang, Yimei, Zweifel, Larry S, Palmiter, Richard D, Storm, Daniel R
Format: Article
Language:English
Subjects:
ADCY3
Adenylyl Cyclases - deficiency
Adenylyl Cyclases - physiology
Animals
Behavior, Animal - physiology
Ciliopathies
Depressive Disorder, Major - enzymology
Depressive Disorder, Major - physiopathology
Disease Models, Animal
Long-Term Potentiation - physiology
Major depressive disorder (MDD)
Mice
Mice, Knockout
Neuronal activity
Phenotype
Primary cilia
Psychiatry
Sleep alteration
Sleep Wake Disorders - physiopathology
Spatial Navigation - physiology
Type III adenylyl cyclase (AC3
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Summary:Abstract Background Although major depressive disorder (MDD) has low heritability, a genome-wide association study in humans has recently implicated type 3 adenylyl cyclase (AC3; ADCY3 ) in MDD. Moreover, the expression level of AC3 in blood has been considered as a MDD biomarker in humans. Nevertheless, there is a lack of supporting evidence from animal studies. Methods We employed multiple approaches to experimentally evaluate if AC3 is a contributing factor for major depression using mouse models lacking the Adcy3 gene. Results We found that conventional AC3 knockout (KO) mice exhibited phenotypes associated with MDD in behavioral assays. Electroencephalography/electromyography recordings indicated that AC3 KO mice have altered sleep patterns characterized by increased percentage of rapid eye movement sleep. AC3 KO mice also exhibit neuronal atrophy. Furthermore, synaptic activity at cornu ammonis 3–cornu ammonis 1 synapses was significantly lower in AC3 KO mice, and they also exhibited attenuated long-term potentiation as well as deficits in spatial navigation. To confirm that these defects are not secondary responses to anosmia or developmental defects, we generated a conditional AC3 floxed mouse strain. This enabled us to inactivate AC3 function selectively in the forebrain and to inducibly ablate it in adult mice. Both AC3 forebrain-specific and AC3 inducible knockout mice exhibited prodepression phenotypes without anosmia. Conclusions This study demonstrates that loss of AC3 in mice leads to decreased neuronal activity, altered sleep pattern, and depression-like behaviors, providing strong evidence supporting AC3 as a contributing factor for MDD.
ISSN:0006-3223
1873-2402
DOI:10.1016/j.biopsych.2015.12.012