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Doublesex and mab-3-related transcription factor 5 promotes midbrain dopaminergic identity in pluripotent stem cells by enforcing a ventral-medial progenitor fate

机译:Doublesex和与mab-3相关的转录因子5通过强制腹侧-内侧祖细胞命运促进多能干细胞中脑多巴胺能的同一性

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摘要

Understanding the control of cell-fate choices during embryonic stem cell (ESC) differentiation is crucial for harnessing strategies for efficient production of desired cell types for pharmaceutical drug screening and cell transplantation. Here we report the identification of the zinc finger-like doublesex and mab-3-related transcription factor 5 (Dmrt5) as a marker for mammalian ventral-medial mesencephalic neuroepithelium that give rise to dopamine neurons. Gain-and loss-of-function studies in ESC demonstrate that Dmrt5 is critically involved in the specification of ventral-medial neural progenitor cell fate and the subsequent generation of dopamine neurons expressing essential midbrain characteristics. Genome-wide analysis of Dmrt5-mediated transcriptome changes and expression profiling of ventral-medial and ventral-lateral mesencephalic neuroepithelium revealed suppressive and inductive regulatory roles for Dmrt5 in the transcription program associated with the ventral-medial neural progenitor fates. Together, these data identify Dmrt5 as an important player in ventral mesencephalic neural fate specification.
机译:了解胚胎干细胞(ESC)分化过程中细胞命运选择的控制对于利用策略有效生产所需细胞类型进行药物筛选和细胞移植至关重要。在这里,我们报告锌指状双性恋和与mab-3相关的转录因子5(Dmrt5)的鉴定,作为哺乳动物腹侧中脑神经上皮上皮细胞的标志物,引起多巴胺神经元。在ESC中进行功能获得和丧失的研究表明,Dmrt5参与了腹侧-中枢神经祖细胞命运的规范以及随后表达多巴胺神经元表达中脑基本特征的过程。 Dmrt5介导的转录组变化的全基因组分析以及腹内侧和腹外侧中脑神经上皮的表达谱分析显示,Dmrt5在与腹内侧神经祖细胞命运相关的转录程序中具有抑制性和诱导性调节作用。总之,这些数据表明Dmrt5是腹侧中脑神经命运规范的重要参与者。

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