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Purkinje cells and Bergmann glia are primary targets of the TRα1 thyroid hormone receptor during mouse cerebellum postnatal development

机译:Purkinje细胞和Bergmann胶质细胞是小鼠小脑出生后TRα1甲状腺激素受体的主要靶标

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摘要

Thyroid hormone is necessary for normal development of the central nervous system, as shown by the severe mental retardation syndrome affecting hypothyroid patients with low levels of active thyroid hormone. The postnatal defects observed in hypothyroid mouse cerebellum are recapitulated in mice heterozygous for a dominant-negative mutation of Thra, the gene encoding the ubiquitous TRα1 receptor. Using CRE/loxP-mediated conditional expression approach, we found that this mutation primarily alters the differentiation of Purkinje cells and Bergmann glia, two cerebellumspecific cell types. These primary defects indirectly affect cerebellum development in a global manner. Notably, the inward migration and terminal differentiation of granule cell precursors is impaired. Therefore, despite the broad distribution of its receptors, thyroid hormone targets few cell types that exert a predominant role in the network of cellular interactions that govern normal cerebellum maturation.
机译:甲状腺激素是中枢神经系统正常发育所必需的,严重的智力低下综合症表明,甲状腺功能低下的甲状腺功能减退患者会受到影响。在甲状腺功能减退小鼠小脑中观察到的产后缺陷在杂合子小鼠中概括为Thra(编码普遍存在的TRα1受体的基因)的显性负突变。使用CRE / loxP介导的条件表达方法,我们发现该突变主要改变了Purkinje细胞和Bergmann胶质细胞这两种小脑特异性细胞类型的分化。这些主要缺陷以整体方式间接影响小脑发育。值得注意的是,颗粒细胞前体的向内迁移和终末分化受到损害。因此,尽管其受体分布广泛,但甲状腺激素靶向的细胞类型却很少,在控制正常小脑成熟的细胞相互作用网络中起主要作用。

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