Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs

MicroRNAs regulate networks of genes to orchestrate cellular functions. MiR-125b, the vertebrate homologue of the Caenorhabditis elegans microRNA lin-4, has been implicated in the regulation of neural and hematopoietic stem cell homeostasis, analogous to how lin-4 regulates stem cells in C. elegans....

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Autores principales: Le, Minh T. N., Shyh-Chang, Ng, Khaw, Swea Ling, Chin, Lingzi, Teh, Cathleen, Tay, Junliang, O'Day, Elizabeth, Korzh, Vladimir, Yang, Henry, Lal, Ashish, Lieberman, Judy, Lodish, Harvey F., Lim, Bing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3174204/
https://www.ncbi.nlm.nih.gov/pubmed/21935352
http://dx.doi.org/10.1371/journal.pgen.1002242
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author Le, Minh T. N.
Shyh-Chang, Ng
Khaw, Swea Ling
Chin, Lingzi
Teh, Cathleen
Tay, Junliang
O'Day, Elizabeth
Korzh, Vladimir
Yang, Henry
Lal, Ashish
Lieberman, Judy
Lodish, Harvey F.
Lim, Bing
author_facet Le, Minh T. N.
Shyh-Chang, Ng
Khaw, Swea Ling
Chin, Lingzi
Teh, Cathleen
Tay, Junliang
O'Day, Elizabeth
Korzh, Vladimir
Yang, Henry
Lal, Ashish
Lieberman, Judy
Lodish, Harvey F.
Lim, Bing
author_sort Le, Minh T. N.
collection PubMed
description MicroRNAs regulate networks of genes to orchestrate cellular functions. MiR-125b, the vertebrate homologue of the Caenorhabditis elegans microRNA lin-4, has been implicated in the regulation of neural and hematopoietic stem cell homeostasis, analogous to how lin-4 regulates stem cells in C. elegans. Depending on the cell context, miR-125b has been proposed to regulate both apoptosis and proliferation. Because the p53 network is a central regulator of both apoptosis and proliferation, the dual roles of miR-125b raise the question of what genes in the p53 network might be regulated by miR-125b. By using a gain- and loss-of-function screen for miR-125b targets in humans, mice, and zebrafish and by validating these targets with the luciferase assay and a novel miRNA pull-down assay, we demonstrate that miR-125b directly represses 20 novel targets in the p53 network. These targets include both apoptosis regulators like Bak1, Igfbp3, Itch, Puma, Prkra, Tp53inp1, Tp53, Zac1, and also cell-cycle regulators like cyclin C, Cdc25c, Cdkn2c, Edn1, Ppp1ca, Sel1l, in the p53 network. We found that, although each miRNA–target pair was seldom conserved, miR-125b regulation of the p53 pathway is conserved at the network level. Our results lead us to propose that miR-125b buffers and fine-tunes p53 network activity by regulating the dose of both proliferative and apoptotic regulators, with implications for tissue stem cell homeostasis and oncogenesis.
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spelling pubmed-31742042011-09-20 Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs Le, Minh T. N. Shyh-Chang, Ng Khaw, Swea Ling Chin, Lingzi Teh, Cathleen Tay, Junliang O'Day, Elizabeth Korzh, Vladimir Yang, Henry Lal, Ashish Lieberman, Judy Lodish, Harvey F. Lim, Bing PLoS Genet Research Article MicroRNAs regulate networks of genes to orchestrate cellular functions. MiR-125b, the vertebrate homologue of the Caenorhabditis elegans microRNA lin-4, has been implicated in the regulation of neural and hematopoietic stem cell homeostasis, analogous to how lin-4 regulates stem cells in C. elegans. Depending on the cell context, miR-125b has been proposed to regulate both apoptosis and proliferation. Because the p53 network is a central regulator of both apoptosis and proliferation, the dual roles of miR-125b raise the question of what genes in the p53 network might be regulated by miR-125b. By using a gain- and loss-of-function screen for miR-125b targets in humans, mice, and zebrafish and by validating these targets with the luciferase assay and a novel miRNA pull-down assay, we demonstrate that miR-125b directly represses 20 novel targets in the p53 network. These targets include both apoptosis regulators like Bak1, Igfbp3, Itch, Puma, Prkra, Tp53inp1, Tp53, Zac1, and also cell-cycle regulators like cyclin C, Cdc25c, Cdkn2c, Edn1, Ppp1ca, Sel1l, in the p53 network. We found that, although each miRNA–target pair was seldom conserved, miR-125b regulation of the p53 pathway is conserved at the network level. Our results lead us to propose that miR-125b buffers and fine-tunes p53 network activity by regulating the dose of both proliferative and apoptotic regulators, with implications for tissue stem cell homeostasis and oncogenesis. Public Library of Science 2011-09-15 /pmc/articles/PMC3174204/ /pubmed/21935352 http://dx.doi.org/10.1371/journal.pgen.1002242 Text en Le T. N. et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Le, Minh T. N.
Shyh-Chang, Ng
Khaw, Swea Ling
Chin, Lingzi
Teh, Cathleen
Tay, Junliang
O'Day, Elizabeth
Korzh, Vladimir
Yang, Henry
Lal, Ashish
Lieberman, Judy
Lodish, Harvey F.
Lim, Bing
Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title_full Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title_fullStr Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title_full_unstemmed Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title_short Conserved Regulation of p53 Network Dosage by MicroRNA–125b Occurs through Evolving miRNA–Target Gene Pairs
title_sort conserved regulation of p53 network dosage by microrna–125b occurs through evolving mirna–target gene pairs
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3174204/
https://www.ncbi.nlm.nih.gov/pubmed/21935352
http://dx.doi.org/10.1371/journal.pgen.1002242
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