Department of Biological Sciences, Tata Institute of Fundamental Research, Mumbai, India.
FASEB J. 2010 Dec;24(12):4793-805. doi: 10.1096/fj.10-161802. Epub 2010 Aug 13.
Thyroid hormone regulates adult hippocampal neurogenesis, a process involved in key functions, such as learning, memory, and mood regulation. We addressed the role of thyroid hormone receptor TRα1 in adult hippocampal neurogenesis, using mice harboring a TRα1 null allele (TRα1(-/-)), overexpressing TRα1 6-fold (TRα2(-/-)), and a mutant TRα1 (TRα1(+/m)) with a 10-fold lower affinity to the ligand. While hippocampal progenitor proliferation was unaltered, TRα1(-/-) mice exhibited a significant increase in doublecortin-positive immature neurons and increased survival of bromodeoxyuridine-positive (BrdU(+)) progenitors as compared to wild-type controls. In contrast, the TRα1(+/m) and the TRα2(-/-) mice, where the overexpressed TRα1 acts as an aporeceptor, showed a significant decline in surviving BrdU(+) progenitors. TRα1(-/-) and TRα2(-/-) mice showed opposing effects on neurogenic markers like polysialylated neural cell adhesion molecule and stathmin. The decreased progenitor survival in the TRα2(-/-) and TRα1(+/m) mice could be rescued by thyroid hormone treatment, as was the decline in neuronal differentiation seen in the TRα1(+/m) mice. These mice also exhibited a decrease in NeuroD(+) cell numbers in the dentate gyrus, suggesting an effect on early postmitotic progenitors. Our results provide the first evidence of a role for unliganded TRα1 in modulating the deleterious effects of hypothyroidism on adult hippocampal neurogenesis.
甲状腺激素调节成年海马神经发生,这一过程涉及学习、记忆和情绪调节等关键功能。我们利用携带甲状腺激素受体 TRα1 缺失等位基因(TRα1(-/-))、6 倍过表达 TRα1(TRα2(-/-))和一种配体结合亲和力降低 10 倍的突变型 TRα1(TRα1(+/m))的小鼠,研究了甲状腺激素受体 TRα1 在成年海马神经发生中的作用。虽然海马祖细胞增殖没有改变,但与野生型对照相比,TRα1(-/-)小鼠双皮质素阳性未成熟神经元数量显著增加,溴脱氧尿苷阳性(BrdU(+))祖细胞存活率增加。相比之下,过表达的 TRα1 作为无配体结合受体的 TRα1(+/m)和 TRα2(-/-)小鼠,其存活的 BrdU(+)祖细胞数量显著减少。TRα1(-/-)和 TRα2(-/-)小鼠在神经发生标志物如多涎酸神经细胞黏附分子和 stathmin 上表现出相反的作用。TRα2(-/-)和 TRα1(+/m)小鼠中祖细胞存活率的降低可以通过甲状腺激素治疗得到挽救,正如在 TRα1(+/m)小鼠中观察到的神经元分化下降一样。这些小鼠还表现出齿状回中 NeuroD(+)细胞数量减少,表明对早期有丝分裂后祖细胞有影响。我们的研究结果首次提供了证据,证明未结合的 TRα1 在调节甲状腺功能减退对成年海马神经发生的有害影响方面发挥作用。