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A modular gain-of-function approach to generate cortical interneuron subtypes from ES cells

机译:一种从ES细胞生成皮质中间神经元亚型的模块化功能增益方法

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Whereas past work indicates that cortical interneurons (cINs) can be generically produced from stem cells, generating large numbers of specific subtypes of this population has remained elusive. This reflects an information gap in our understanding of the transcriptional programs required for different interneuron subtypes. Here, we have utilized the directed differentiation of stem cells into specific subpopulations of cortical interneurons as a means to identify some of these missing factors. To establish this approach, we utilized two factors known to be required for the generation of cINs, Nkx2-1 and Dlx2. As predicted, their regulated transient expression greatly improved the differentiation efficiency and specificity over baseline. We extended upon this "cIN-primed" model in order to establish a modular system whereby a third transcription factor could be systematically introduced. Using this approach, we identified Lmo3 and Pou3f4 as genes that can augment the differentiation and/or subtype specificity of cINs invitro.
机译:过去的研究表明,皮质干神经元(cIN)可以从干细胞中普遍产生,而产生大量特定亚型的人仍然难以捉摸。这反映了我们对不同中间神经元亚型所需的转录程序的理解上的信息鸿沟。在这里,我们已经利用干细胞定向分化为皮质中间神经元的特定亚群,作为鉴定这些缺失因子中某些的手段。为了建立这种方法,我们利用了两个已知的cIN生成所需的因子Nkx2-1和Dlx2。如所预测的,它们调控的瞬时表达大大提高了分化效率和特异性。我们扩展了这种“ cIN启动”模型,以便建立一个模块化系统,从而可以系统地引入第三个转录因子。使用这种方法,我们确定Lmo3和Pou3f4为可以增强cINs体外分化和/或亚型特异性的基因。

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