Identification of TGFβ signaling as a regulator of interneuron neurogenesis in a human pluripotent stem cell model.

Q4 Neuroscience
Neuronal signaling Pub Date : 2021-12-07 eCollection Date: 2021-12-01 DOI:10.1042/NS20210020
Maria Santos Cruz, Meng Li
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引用次数: 2

Abstract

Cortical interneurons are GABAergic inhibitory cells that connect locally in the neocortex and play a pivotal role in shaping cortical network activities. Dysfunction of these cells is believed to lead to runaway excitation underlying seizure-based diseases, such as epilepsy, autism and schizophrenia. There is a growing interest in using cortical interneurons derived from human pluripotent stem cells for understanding their complex development and for modeling neuropsychiatric diseases. Here, we report the identification of a novel role of transforming growth factor β (TGFβ) signaling in modulating interneuron progenitor maintenance and neuronal differentiation. TGFβ signaling inhibition suppresses terminal differentiation of interneuron progenitors, while exogenous TGFβ3 accelerates the transition of progenitors into postmitotic neurons. We provide evidence that TGFb signaling exerts this function via regulating cell cycle length of the NKX2.1+ neural progenitors. Together, the present study represents a useful platform for studying human interneuron development and interneuron-associated neurological diseases with human pluripotent stem cells.

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在人多能干细胞模型中tgf - β信号作为中间神经元神经发生调节因子的鉴定。
皮层中间神经元是gaba能抑制细胞,在新皮层局部连接,在形成皮层网络活动中起关键作用。这些细胞的功能障碍被认为会导致癫痫、自闭症和精神分裂症等癫痫性疾病的失控兴奋。人们对利用来自人类多能干细胞的皮质中间神经元来了解其复杂的发育和神经精神疾病的建模越来越感兴趣。在这里,我们报告了转化生长因子β (TGFβ)信号在调节中间神经元祖细胞维持和神经元分化中的新作用。tgf - β信号抑制抑制中间神经元祖细胞的终末分化,而外源tgf - β3加速祖细胞向有丝分裂后神经元的转变。我们提供的证据表明,TGFb信号通过调节NKX2.1+神经祖细胞的细胞周期长度来发挥这一功能。总之,本研究为人类多能干细胞研究人类中间神经元发育和中间神经元相关神经系统疾病提供了一个有用的平台。
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来源期刊
CiteScore
4.60
自引率
0.00%
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审稿时长
14 weeks
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