| Literature DB >> 33684100 |
John P Zepecki1, David Karambizi1, J Eduardo Fajardo2, Kristin M Snyder3, Charlotte Guetta-Terrier1, Oliver Y Tang1, Jia-Shu Chen1, Atom Sarkar4, Andras Fiser2, Steven A Toms5, Nikos Tapinos1,5,6,7.
Abstract
Within the glioblastoma cellular niche, glioma stem cells (GSCs) can give rise to differentiated glioma cells (DGCs) and, when necessary, DGCs can reciprocally give rise to GSCs to maintain the cellular equilibrium necessary for optimal tumor growth. Here, using ribosome profiling, transcriptome and m6A RNA sequencing, we show that GSCs from patients with different subtypes of glioblastoma share a set of transcripts, which exhibit a pattern of m6A loss and increased protein translation during differentiation. The target sequences of a group of miRNAs overlap the canonical RRACH m6A motifs of these transcripts, many of which confer a survival advantage in glioblastoma. Ectopic expression of the RRACH-binding miR-145 induces loss of m6A, formation of FTO/AGO1/ILF3/miR-145 complexes on a clinically relevant tumor suppressor gene (CLIP3) and significant increase in its nascent translation. Inhibition of miR-145 maintains RRACH m6A levels of CLIP3 and inhibits its nascent translation. This study highlights a critical role of miRNAs in assembling complexes for m6A demethylation and induction of protein translation during GSC state transition.Entities:
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Year: 2021 PMID: 33684100 PMCID: PMC7971852 DOI: 10.1371/journal.pgen.1009086
Source DB: PubMed Journal: PLoS Genet ISSN: 1553-7390 Impact factor: 6.020