生物
神经干细胞
祖细胞
神经细胞
神经发育
神经科学
细胞分化
阿尔法(金融)
细胞
细胞命运测定
干细胞
细胞生物学
遗传学
基因
转录因子
护理部
医学
患者满意度
结构效度
作者
Matti Lam,Mohsen Moslem,Julien Bryois,Robin Pronk,Elias Uhlin,Ivar Dehnisch Ellström,Loora Laan,Jessica Olive,Rebecca S. Morse,Harriet Rönnholm,Lauri Louhivuori,Sergiy V. Korol,Niklas Dahl,Per Uhlén,Britt‐Marie Anderlid,Malin Kele,Patrick F. Sullivan,Anna Falk
标识
DOI:10.1016/j.yexcr.2019.06.014
摘要
We generated human iPS derived neural stem cells and differentiated cells from healthy control individuals and an individual with autism spectrum disorder carrying bi-allelic NRXN1-alpha deletion. We investigated the expression of NRXN1-alpha during neural induction and neural differentiation and observed a pivotal role for NRXN1-alpha during early neural induction and neuronal differentiation. Single cell RNA-seq pinpointed neural stem cells carrying NRXN1-alpha deletion shifting towards radial glia-like cell identity and revealed higher proportion of differentiated astroglia. Furthermore, neuronal cells carrying NRXN1-alpha deletion were identified as immature by single cell RNA-seq analysis, displayed significant depression in calcium signaling activity and presented impaired maturation action potential profile in neurons investigated with electrophysiology. Our observations propose NRXN1-alpha plays an important role for the efficient establishment of neural stem cells, in neuronal differentiation and in maturation of functional excitatory neuronal cells.
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