Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options

During the past decade, the age-adjusted mortality rate for endometrial cancer (EC) increased 1.9% annually with TP53 mutant (TP53-mu) EC disproportionally represented in advanced disease and deaths. Therefore, we aimed to assess pivotal molecular parameters that differentiate clinical outcomes in h...

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Autores principales: Bosquet, Jesus Gonzalez, Zhang, Qing, Cliby, William A., Bakkum-Gamez, Jamie N., Cen, Ling, Dowdy, Sean C., Sherman, Mark E., Weroha, S. John, Clayton, Amy C., Kipp, Benjamin R., Halling, Kevin C., Couch, Fergus J., Podratz, Karl C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7840025/
https://www.ncbi.nlm.nih.gov/pubmed/33503056
http://dx.doi.org/10.1371/journal.pone.0245664
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author Bosquet, Jesus Gonzalez
Zhang, Qing
Cliby, William A.
Bakkum-Gamez, Jamie N.
Cen, Ling
Dowdy, Sean C.
Sherman, Mark E.
Weroha, S. John
Clayton, Amy C.
Kipp, Benjamin R.
Halling, Kevin C.
Couch, Fergus J.
Podratz, Karl C.
author_facet Bosquet, Jesus Gonzalez
Zhang, Qing
Cliby, William A.
Bakkum-Gamez, Jamie N.
Cen, Ling
Dowdy, Sean C.
Sherman, Mark E.
Weroha, S. John
Clayton, Amy C.
Kipp, Benjamin R.
Halling, Kevin C.
Couch, Fergus J.
Podratz, Karl C.
author_sort Bosquet, Jesus Gonzalez
collection PubMed
description During the past decade, the age-adjusted mortality rate for endometrial cancer (EC) increased 1.9% annually with TP53 mutant (TP53-mu) EC disproportionally represented in advanced disease and deaths. Therefore, we aimed to assess pivotal molecular parameters that differentiate clinical outcomes in high- and low-risk EC. Using the Cancer Genome Atlas, we analyzed EC specimens with available DNA sequences and quantitative gene-specific RNA expression data. After polymerase ɛ (POLE)-mutant specimens were excluded, differential gene-specific mutations and mRNA expressions were annotated and integrated. Consequent to TP53-mu failure to induce p21, derepression of multiple oncogenes harboring promoter p21 repressive sites was observed, including CCNA2 and FOXM1 (P < .001 compared with TP53 wild type [TP53-wt]). TP53-wt EC with high CCNA2 expression (CCNA2-H) had a targeted transcriptomic profile similar to that of TP53-mu EC, suggesting CCNA2 is a seminal determinant for both TP53-wt and TP53-mu EC. CCNA2 enhances E2F1 function, upregulating FOXM1 and CIP2A, as observed in TP53-mu and CCNA2-H TP53-wt EC (P < .001). CIP2A inhibits protein phosphatase 2A, leading to AKT inactivation of GSK3β and restricted oncoprotein degradation; PPP2R1A and FBXW7 mutations yield similar results. Upregulation of FOXM1 and failed degradation of FOXM1 is evidenced by marked upregulation of multiple homologous recombination genes (P < .001). Integrating these molecular aberrations generated a molecular biomarker panel with significant prognostic discrimination (P = 5.8×10(−7)); adjusting for age, histology, grade, myometrial invasion, TP53 status, and stage, only CCNA2-H/E2F1-H (P = .0003), FBXW7-mu/PPP2R1A-mu (P = .0002), and stage (P = .017) were significant. The generated prognostic molecular classification system identifies dissimilar signaling aberrations potentially amenable to targetable therapeutic options.
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spelling pubmed-78400252021-02-02 Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options Bosquet, Jesus Gonzalez Zhang, Qing Cliby, William A. Bakkum-Gamez, Jamie N. Cen, Ling Dowdy, Sean C. Sherman, Mark E. Weroha, S. John Clayton, Amy C. Kipp, Benjamin R. Halling, Kevin C. Couch, Fergus J. Podratz, Karl C. PLoS One Research Article During the past decade, the age-adjusted mortality rate for endometrial cancer (EC) increased 1.9% annually with TP53 mutant (TP53-mu) EC disproportionally represented in advanced disease and deaths. Therefore, we aimed to assess pivotal molecular parameters that differentiate clinical outcomes in high- and low-risk EC. Using the Cancer Genome Atlas, we analyzed EC specimens with available DNA sequences and quantitative gene-specific RNA expression data. After polymerase ɛ (POLE)-mutant specimens were excluded, differential gene-specific mutations and mRNA expressions were annotated and integrated. Consequent to TP53-mu failure to induce p21, derepression of multiple oncogenes harboring promoter p21 repressive sites was observed, including CCNA2 and FOXM1 (P < .001 compared with TP53 wild type [TP53-wt]). TP53-wt EC with high CCNA2 expression (CCNA2-H) had a targeted transcriptomic profile similar to that of TP53-mu EC, suggesting CCNA2 is a seminal determinant for both TP53-wt and TP53-mu EC. CCNA2 enhances E2F1 function, upregulating FOXM1 and CIP2A, as observed in TP53-mu and CCNA2-H TP53-wt EC (P < .001). CIP2A inhibits protein phosphatase 2A, leading to AKT inactivation of GSK3β and restricted oncoprotein degradation; PPP2R1A and FBXW7 mutations yield similar results. Upregulation of FOXM1 and failed degradation of FOXM1 is evidenced by marked upregulation of multiple homologous recombination genes (P < .001). Integrating these molecular aberrations generated a molecular biomarker panel with significant prognostic discrimination (P = 5.8×10(−7)); adjusting for age, histology, grade, myometrial invasion, TP53 status, and stage, only CCNA2-H/E2F1-H (P = .0003), FBXW7-mu/PPP2R1A-mu (P = .0002), and stage (P = .017) were significant. The generated prognostic molecular classification system identifies dissimilar signaling aberrations potentially amenable to targetable therapeutic options. Public Library of Science 2021-01-27 /pmc/articles/PMC7840025/ /pubmed/33503056 http://dx.doi.org/10.1371/journal.pone.0245664 Text en © 2021 Bosquet 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 (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.
spellingShingle Research Article
Bosquet, Jesus Gonzalez
Zhang, Qing
Cliby, William A.
Bakkum-Gamez, Jamie N.
Cen, Ling
Dowdy, Sean C.
Sherman, Mark E.
Weroha, S. John
Clayton, Amy C.
Kipp, Benjamin R.
Halling, Kevin C.
Couch, Fergus J.
Podratz, Karl C.
Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title_full Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title_fullStr Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title_full_unstemmed Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title_short Association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
title_sort association of a novel endometrial cancer biomarker panel with prognostic risk, platinum insensitivity, and targetable therapeutic options
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7840025/
https://www.ncbi.nlm.nih.gov/pubmed/33503056
http://dx.doi.org/10.1371/journal.pone.0245664
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