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Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma

MicroRNA (miRNA)-based therapies are an emerging class of targeted therapeutics with many potential applications. Ewing Sarcoma patients could benefit dramatically from personalized miRNA therapy due to inter-patient heterogeneity and a lack of druggable (to this point) targets. However, because of...

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Autores principales: Weaver, Davis T., Pishas, Kathleen I., Williamson, Drew, Scarborough, Jessica, Lessnick, Stephen L., Dhawan, Andrew, Scott, Jacob G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8601628/
https://www.ncbi.nlm.nih.gov/pubmed/34662337
http://dx.doi.org/10.1371/journal.pcbi.1008755
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author Weaver, Davis T.
Pishas, Kathleen I.
Williamson, Drew
Scarborough, Jessica
Lessnick, Stephen L.
Dhawan, Andrew
Scott, Jacob G.
author_facet Weaver, Davis T.
Pishas, Kathleen I.
Williamson, Drew
Scarborough, Jessica
Lessnick, Stephen L.
Dhawan, Andrew
Scott, Jacob G.
author_sort Weaver, Davis T.
collection PubMed
description MicroRNA (miRNA)-based therapies are an emerging class of targeted therapeutics with many potential applications. Ewing Sarcoma patients could benefit dramatically from personalized miRNA therapy due to inter-patient heterogeneity and a lack of druggable (to this point) targets. However, because of the broad effects miRNAs may have on different cells and tissues, trials of miRNA therapies have struggled due to severe toxicity and unanticipated immune response. In order to overcome this hurdle, a network science-based approach is well-equipped to evaluate and identify miRNA candidates and combinations of candidates for the repression of key oncogenic targets while avoiding repression of essential housekeeping genes. We first characterized 6 Ewing sarcoma cell lines using mRNA sequencing. We then estimated a measure of tumor state, which we term network potential, based on both the mRNA gene expression and the underlying protein-protein interaction network in the tumor. Next, we ranked mRNA targets based on their contribution to network potential. We then identified miRNAs and combinations of miRNAs that preferentially act to repress mRNA targets with the greatest influence on network potential. Our analysis identified TRIM25, APP, ELAV1, RNF4, and HNRNPL as ideal mRNA targets for Ewing sarcoma therapy. Using predicted miRNA-mRNA target mappings, we identified miR-3613-3p, let-7a-3p, miR-300, miR-424-5p, and let-7b-3p as candidate optimal miRNAs for preferential repression of these targets. Ultimately, our work, as exemplified in the case of Ewing sarcoma, describes a novel pipeline by which personalized miRNA cocktails can be designed to maximally perturb gene networks contributing to cancer progression.
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spelling pubmed-86016282021-11-19 Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma Weaver, Davis T. Pishas, Kathleen I. Williamson, Drew Scarborough, Jessica Lessnick, Stephen L. Dhawan, Andrew Scott, Jacob G. PLoS Comput Biol Research Article MicroRNA (miRNA)-based therapies are an emerging class of targeted therapeutics with many potential applications. Ewing Sarcoma patients could benefit dramatically from personalized miRNA therapy due to inter-patient heterogeneity and a lack of druggable (to this point) targets. However, because of the broad effects miRNAs may have on different cells and tissues, trials of miRNA therapies have struggled due to severe toxicity and unanticipated immune response. In order to overcome this hurdle, a network science-based approach is well-equipped to evaluate and identify miRNA candidates and combinations of candidates for the repression of key oncogenic targets while avoiding repression of essential housekeeping genes. We first characterized 6 Ewing sarcoma cell lines using mRNA sequencing. We then estimated a measure of tumor state, which we term network potential, based on both the mRNA gene expression and the underlying protein-protein interaction network in the tumor. Next, we ranked mRNA targets based on their contribution to network potential. We then identified miRNAs and combinations of miRNAs that preferentially act to repress mRNA targets with the greatest influence on network potential. Our analysis identified TRIM25, APP, ELAV1, RNF4, and HNRNPL as ideal mRNA targets for Ewing sarcoma therapy. Using predicted miRNA-mRNA target mappings, we identified miR-3613-3p, let-7a-3p, miR-300, miR-424-5p, and let-7b-3p as candidate optimal miRNAs for preferential repression of these targets. Ultimately, our work, as exemplified in the case of Ewing sarcoma, describes a novel pipeline by which personalized miRNA cocktails can be designed to maximally perturb gene networks contributing to cancer progression. Public Library of Science 2021-10-18 /pmc/articles/PMC8601628/ /pubmed/34662337 http://dx.doi.org/10.1371/journal.pcbi.1008755 Text en © 2021 Weaver et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Weaver, Davis T.
Pishas, Kathleen I.
Williamson, Drew
Scarborough, Jessica
Lessnick, Stephen L.
Dhawan, Andrew
Scott, Jacob G.
Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title_full Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title_fullStr Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title_full_unstemmed Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title_short Network potential identifies therapeutic miRNA cocktails in Ewing sarcoma
title_sort network potential identifies therapeutic mirna cocktails in ewing sarcoma
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8601628/
https://www.ncbi.nlm.nih.gov/pubmed/34662337
http://dx.doi.org/10.1371/journal.pcbi.1008755
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