4.3 Article

Behavioral and gene expression analyse mice as a possible animal model of of Wfs1 knockout mice as a possible animal model moods disorder

Journal

NEUROSCIENCE RESEARCH
Volume 61, Issue 2, Pages 143-158

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.neures.2008.02.002

Keywords

Wolframin; Wolfram disease; depression; bipolar disorder; DNA microarray; forced swimming test

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Wolfram disease is a rare genetic disorder frequently accompanying depression and psychosis. Non-symptomatic mutation carriers also have higher rates of depression and suicide. Because WfS1, the causative gene of Wolfram disease, is located at 4p16, a linkage locus for bipolar disorder, mutations of WfS1 were suggested to be involved in the pathophysiology of bipolar disorder. In this study, we performed behavioral and gene expression analyses of Wfs1 knockout mice to assess the validity as an animal model of mood disorder. In addition, the distribution of Wfs1 protein was examined in mouse brain. Wfs1 knockout mice did not show abnormalities in circadian rhythm and periodic fluctuation of wheel-running activity. Behavioral analysis showed that Wfs1 knockout mice had retardation in emotionally triggered behavior, decreased social interaction, and altered behavioral despair depending on experimental conditions. Wfs1-like immunoreactivity inmouse brain showed a similar distribution pattern to that in rats, including several nuclei potentially relevant to the symptoms of mood disorders. Gene expression analysis showed down-regulation of Cdc42ep5 and Rnd1, both of which are related to Rho GTPase, which plays a role in dendrite development. These findings may be relevant to the mood disorder observed in patients with Wolfram disease. (c) 2008 Published by Elsevier Ireland Ltd and the Japan Neuroscience Society.

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