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Cortical interneurons from human pluripotent stem cells: prospects for neurological and psychiatric disease

机译:人类多能干细胞的皮质中间神经元:神经病学和精神病学的前景

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摘要

Cortical interneurons represent 20% of the cells in the cortex. These cells are local inhibitory neurons whose function is to modulate the firing activities of the excitatory projection neurons. Cortical interneuron dysfunction is believed to lead to runaway excitation underlying (or implicated in) seizure-based diseases, such as epilepsy, autism, and schizophrenia. The complex development of this cell type and the intricacies involved in defining the relative subtypes are being increasingly well defined. This has led to exciting experimental cell therapy in model organisms, whereby fetal-derived interneuron precursors can reverse seizure severity and reduce mortality in adult epileptic rodents. These proof-of-principle studies raise hope for potential interneuron-based transplantation therapies for treating epilepsy. On the other hand, cortical neurons generated from patient iPSCs serve as a valuable tool to explore genetic influences of interneuron development and function. This is a fundamental step in enhancing our understanding of the molecular basis of neuropsychiatric illnesses and the development of targeted treatments. Protocols are currently being developed for inducing cortical interneuron subtypes from mouse and human pluripotent stem cells. This review sets out to summarize the progress made in cortical interneuron development, fetal tissue transplantation and the recent advance in stem cell differentiation toward interneurons.
机译:皮质中间神经元代表皮质中20%的细胞。这些细胞是局部抑制性神经元,其功能是调节兴奋性投射神经元的激发活性。据信皮质中神经元功能障碍导致基于癫痫发作的疾病(例如癫痫,自闭症和精神分裂症)的失控激发(或与之相关)。这种细胞类型的复杂发展以及定义相对亚型所涉及的复杂性越来越好地被定义。这导致了在模型生物中令人兴奋的实验性细胞疗法,其中胎儿来源的中间神经元前体可以逆转癫痫发作的严重程度并降低成年癫痫鼠的死亡率。这些原理验证研究为潜在的基于中间神经元的移植疗法治疗癫痫病带来了希望。另一方面,从患者iPSC产生的皮质神经元可作为探索中间神经元发育和功能的遗传影响的宝贵工具。这是增进我们对神经精神疾病的分子基础和靶向治疗的理解的基本步骤。目前正在开发用于从小鼠和人多能干细胞中诱导皮质中间神经元亚型的方案。这篇综述着手总结了皮质神经元发育,胎儿组织移植以及干细胞向神经元分化的最新进展。

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