首页> 外文期刊>Behavioural Brain Research: An International Journal >Increased depressive behaviour in mice harboring the mutant thyroid hormone receptor alpha 1.
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Increased depressive behaviour in mice harboring the mutant thyroid hormone receptor alpha 1.

机译:携带突变型甲状腺激素受体α1的小鼠的抑郁行为增加。

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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.
机译:临床证据表明甲状腺功能减退会导致情绪障碍。本研究测试了导致大脑中受体介导的甲状腺功能减退的突变甲状腺激素受体α1(TRalpha1)是否会影响小鼠的抑郁和焦虑行为。对TRalpha1等位基因(TRalpha1 + / m)杂合的小鼠产生与三碘甲状腺素(T3)的亲和力降低了10倍的受体蛋白,并对野生型(wt)小鼠进行了几种范式的测试,它们分别测试了抑郁和焦虑行为。突变小鼠和wt小鼠用T3或溶媒处理。与wt小鼠相比,未经治疗的TRalpha1 + / m动物表现出运动减少,穿梭箱中较高的无助率,惊吓反应中的焦虑水平较高以及暗灯箱行为范例。连续的T3替代疗法可有效缓解焦虑和抑郁行为,而不会影响突变小鼠的运动。值得注意的是,与未经治疗的wt小鼠相比,连续的T3替代降低了wt小鼠的整体运动能力并增加了其无助行为。数据表明,由未配体的甲状腺激素受体α1引起的受体介导的甲状腺功能减退症在小鼠中导致抑郁和焦虑的表型,这对连续的T3取代有反应,并且通过连续的T3给药引起的医源性甲状腺功能亢进症会导致机车不足和抑郁的表型。

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