Behavioral Alterations in Mice Carrying Homozygous <i>HDAC4</i> <sup><i>A778T</i></sup> Missense Mutation Associated With Eating Disorder.
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Abstract |
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Eating disorders (EDs) are serious mental illnesses thought to arise from the complex gene-environment interactions. DNA methylation patterns in histone deacetylase 4 () locus have been associated with EDs and we have previously identified a missense mutation in the gene ( ) that increases the risk of developing an ED. In order to evaluate the biological consequences of this variant and establish a useful mouse model of EDs, here we performed behavioral characterization of mice homozygous for (corresponding to human ) that were further backcrossed onto C57BL/6 background. When fed high-fat diet, male, but not female, homozygous mice showed a trend toward decreased weight gain compared to their wild-type littermates. Behaviorally, male, but not female, homozygous mice spent less time in eating and exhibited reduced motivation to work for palatable food and light phase-specific decrease in locomotor activity. Additionally, homozygous female, but not male, mice display social subordination when subjected to a tube dominance test. Collectively, these results reveal a complex sex- and circadian-dependent role of ED-associated mutation in affecting mouse behaviors. Homozygous mice could therefore be a useful animal model to gain insight into the neurobiological basis of EDs. |
Year of Publication |
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0
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Journal |
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Frontiers in neuroscience
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Volume |
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14
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Number of Pages |
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139
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Date Published |
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2020
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ISSN Number |
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1662-4548
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URL |
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https://doi.org/10.3389/fnins.2020.00139
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DOI |
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10.3389/fnins.2020.00139
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Short Title |
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Front Neurosci
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