| Literature DB >> 27565344 |
Xiaochang Zhang1, Ming Hui Chen2, Xuebing Wu3, Andrew Kodani4, Jean Fan5, Ryan Doan6, Manabu Ozawa7, Jacqueline Ma8, Nobuaki Yoshida7, Jeremy F Reiter4, Douglas L Black9, Peter V Kharchenko5, Phillip A Sharp10, Christopher A Walsh11.
Abstract
Alternative splicing is prevalent in the mammalian brain. To interrogate the functional role of alternative splicing in neural development, we analyzed purified neural progenitor cells (NPCs) and neurons from developing cerebral cortices, revealing hundreds of differentially spliced exons that preferentially alter key protein domains-especially in cytoskeletal proteins-and can harbor disease-causing mutations. We show that Ptbp1 and Rbfox proteins antagonistically govern the NPC-to-neuron transition by regulating neuron-specific exons. Whereas Ptbp1 maintains apical progenitors partly through suppressing a poison exon of Flna in NPCs, Rbfox proteins promote neuronal differentiation by switching Ninein from a centrosomal splice form in NPCs to a non-centrosomal isoform in neurons. We further uncover an intronic human mutation within a PTBP1-binding site that disrupts normal skipping of the FLNA poison exon in NPCs and causes a brain-specific malformation. Our study indicates that dynamic control of alternative splicing governs cell fate in cerebral cortical development.Entities:
Keywords: Ninein; Ptbp1; Rbfox; filamin A; microcephaly; mother centriole; periventricular nodular heterotopia
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Year: 2016 PMID: 27565344 PMCID: PMC5248659 DOI: 10.1016/j.cell.2016.07.025
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582