| Literature DB >> 29719248 |
Akihide Takeuchi1, Kei Iida2, Toshiaki Tsubota3, Motoyasu Hosokawa3, Masatsugu Denawa4, J B Brown5, Kensuke Ninomiya3, Mikako Ito6, Hiroshi Kimura7, Takaya Abe8, Hiroshi Kiyonari9, Kinji Ohno6, Masatoshi Hagiwara10.
Abstract
Genes specifically expressed in neurons contain members with extended long introns. Longer genes present a problem with respect to fulfilment of gene length transcription, and evidence suggests that dysregulation of long genes is a mechanism underlying neurodegenerative and psychiatric disorders. Here, we report the discovery that RNA-binding protein Sfpq is a critical factor for maintaining transcriptional elongation of long genes. We demonstrate that Sfpq co-transcriptionally binds to long introns and is required for sustaining long-gene transcription by RNA polymerase II through mediating the interaction of cyclin-dependent kinase 9 with the elongation complex. Phenotypically, Sfpq disruption caused neuronal apoptosis in developing mouse brains. Expression analysis of Sfpq-regulated genes revealed specific downregulation of developmentally essential neuronal genes longer than 100 kb in Sfpq-disrupted brains; those genes are enriched in associations with neurodegenerative and psychiatric diseases. The identified molecular machinery yields directions for targeted investigations of the association between long-gene transcriptopathy and neuronal diseases.Entities:
Keywords: RBP/transcript-dependent elongation; RNA polymerase II; RNA-binding protein; cyclin-dependent kinase 9; long genopathies; long-gene diseases; long-gene transcriptotherapy; neurological and psychiatric diseases; neuronal development; transcriptional regulation
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Year: 2018 PMID: 29719248 DOI: 10.1016/j.celrep.2018.03.141
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423