AI Article Synopsis
- Clinical evidence shows that hypothyroidism is linked to mood disorders, prompting the study of the impact of a mutant thyroid hormone receptor (TRalpha1) on depression and anxiety in mice.
- Mice with the TRalpha1 mutation exhibited more depressive and anxious behaviors compared to wildtype (wt) mice, especially when untreated, highlighting the role of this receptor in mood regulation.
- Continuous treatment with triiodothyronine (T3) helped alleviate anxiety and depression in the mutant mice, while it negatively impacted locomotion and increased helplessness in the wt mice, suggesting a complex interaction between thyroid hormone levels and mood behaviors.
Article Abstract
Clinical evidence indicates that hypothyroidism contributes to mood disorders. The present study tested if the mutant thyroid hormone receptor alpha 1 (TRalpha1) that causes a receptor-mediated hypothyroidism in the brain affects depressive and anxious behaviour in mice. Mice heterozygous for the TRalpha1 allele (TRalpha1+/m), yielding a receptor protein with a 10-fold reduced affinity to triiodothyronine (T3), and wildtype (wt) mice were subjected to several paradigms specifically testing depressive and anxious behaviour. Mutant and wt mice were either treated with T3 or vehicle. Untreated TRalpha1+/m animals displayed reduced locomotion, higher rates of helplessness in the shuttle box-, greater levels of anxiety in the startle response- and dark light box behavioural paradigms when compared to wt mice. Continuous T3-substitution therapy was effective in alleviating anxious and depressive behaviour without affecting locomotion in mutant mice. Notably, continuous T3-substitution reduced overall locomotion and increased helpless behaviour in wt mice when compared to untreated wt mice. The data suggest that receptor-mediated hypothyroidism caused by an unliganded thyroid hormone receptor alpha 1 leads to a depressive and anxious phenotype in mice, which is responsive to continuous T3-substitution and that an iatrogeneously induced hyperthyreoidism by continuous T3-administration leads to a hypolocomotive and depressive phenotype.
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| http://dx.doi.org/10.1016/j.bbr.2010.05.016 | DOI Listing |
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