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p53 Represses the Oncogenic Sno-MiR-28 Derived from a SnoRNA

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posted on 2024-07-12, 11:41 authored by Feng Yu, Cameron P. Bracken, Katherine A. Pillman, David M. Lawrence, Gregory J. Goodall, David F. Callen, Paul M. Neilsen
p53 is a master tumour repressor that participates in vast regulatory networks, including feedback loops involving microRNAs (miRNAs) that regulate p53 and that themselves are direct p53 transcriptional targets. We show here that a group of polycistronic miRNA-like non-coding RNAs derived from small nucleolar RNAs (sno-miRNAs) are transcriptionally repressed by p53 through their host gene, SNHG1. The most abundant of these, sno-miR-28, directly targets the p53-stabilizing gene, TAF9B. Collectively, p53, SNHG1, sno-miR-28 and TAF9B form a regulatory loop which affects p53 stability and downstream p53-regulated pathways. In addition, SNHG1, SNORD28 and sno-miR-28 are all significantly upregulated in breast tumours and the overexpression of sno-miR-28 promotes breast epithelial cell proliferation. This research has broadened our knowledge of the crosstalk between small non-coding RNA pathways and roles of sno-miRNAs in p53 regulation.

Funding

44112162:NHMRC

Targets of epithelial microRNAs

National Health and Medical Research Council

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ISSN

1932-6203

Journal title

PLoS One

Volume

10

Issue

6

Article number

article no. e0129190

Publisher

Public Library of Science

Copyright statement

Copyright © 2015 Yu et al. This an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Language

eng

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