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Get Free AccessTranscribed ultraconserved regions (T-UCRs) are noncoding RNAs derived from DNA sequences that are entirely conserved across species. Their expression is altered in many tumor types, and, although a role for T-UCRs as regulators of gene expression has been proposed, their functions remain largely unknown. Herein, we describe the epigenetic silencing of the uc.160+ T-UCR in gliomas and mechanistically define a novel RNA-RNA regulatory network in which uc.160+ modulates the biogenesis of several members of the miR-376 cluster. This includes the positive regulation of primary microRNA (pri-miRNA) cleavage and an enhanced A-to-I editing on its mature sequence. As a consequence, the expression of uc.160+ affects the downstream, miR-376-regulated genes, including the transcriptional coregulators RING1 and YY1-binding protein (RYBP) and forkhead box P2 (FOXP2). Finally, we elucidate the clinical impact of our findings, showing that hypermethylation of the uc.160+ CpG island is an independent prognostic factor associated with better overall survival in lower-grade gliomas, highlighting the importance of T-UCRs in cancer pathophysiology.
Marta Soler, Verónica Dávalos, Anaís Sánchez‐Castillo, Carlos Mora‐Martínez, Fernando Setién, Edilene Siqueira Soares, Manuel Castro de Moura, Manel Esteller, Sònia Guil (2021). The transcribed ultraconserved region <i>uc.160+</i> enhances processing and A‐to‐I editing of the <i>miR‐376</i> cluster: hypermethylation improves glioma prognosis. , 16(3), DOI: https://doi.org/10.1002/1878-0261.13121.
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Type
Article
Year
2021
Authors
9
Datasets
0
Total Files
0
Language
en
DOI
https://doi.org/10.1002/1878-0261.13121
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