Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines

To improve our understanding of ovarian cancer, we performed genome-wide analyses of 45 ovarian cancer cell lines. Given the challenges of genomic analyses of tumors without matched normal samples, we developed approaches for detection of somatic sequence and structural changes and integrated these...

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Autores principales: Papp, Eniko, Hallberg, Dorothy, Konecny, Gottfried E., Bruhm, Daniel C., Adleff, Vilmos, Noë, Michaël, Kagiampakis, Ioannis, Palsgrove, Doreen, Conklin, Dylan, Kinose, Yasuto, White, James R., Press, Michael F., Drapkin, Ronny, Easwaran, Hariharan, Baylin, Stephen B., Slamon, Dennis, Velculescu, Victor E., Scharpf, Robert B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6481945/
https://www.ncbi.nlm.nih.gov/pubmed/30485824
http://dx.doi.org/10.1016/j.celrep.2018.10.096
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author Papp, Eniko
Hallberg, Dorothy
Konecny, Gottfried E.
Bruhm, Daniel C.
Adleff, Vilmos
Noë, Michaël
Kagiampakis, Ioannis
Palsgrove, Doreen
Conklin, Dylan
Kinose, Yasuto
White, James R.
Press, Michael F.
Drapkin, Ronny
Easwaran, Hariharan
Baylin, Stephen B.
Slamon, Dennis
Velculescu, Victor E.
Scharpf, Robert B.
author_facet Papp, Eniko
Hallberg, Dorothy
Konecny, Gottfried E.
Bruhm, Daniel C.
Adleff, Vilmos
Noë, Michaël
Kagiampakis, Ioannis
Palsgrove, Doreen
Conklin, Dylan
Kinose, Yasuto
White, James R.
Press, Michael F.
Drapkin, Ronny
Easwaran, Hariharan
Baylin, Stephen B.
Slamon, Dennis
Velculescu, Victor E.
Scharpf, Robert B.
author_sort Papp, Eniko
collection PubMed
description To improve our understanding of ovarian cancer, we performed genome-wide analyses of 45 ovarian cancer cell lines. Given the challenges of genomic analyses of tumors without matched normal samples, we developed approaches for detection of somatic sequence and structural changes and integrated these with epigenetic and expression alterations. Alterations not previously implicated in ovarian cancer included amplification or overexpression of ASXL1 and H3F3B, deletion or underexpression of CDC73 and TGF-beta receptor pathway members, and rearrangements of YAP1-MAML2 and IKZF2-ERBB4. Dose-response analyses to targeted therapies revealed unique molecular dependencies, including increased sensitivity of tumors with PIK3CA and PPP2R1A alterations to PI3K inhibitor GNE-493, MYC amplifications to PARP inhibitor BMN673, and SMAD3/4 alterations to MEK inhibitor MEK162. Genome-wide rearrangements provided an improved measure of sensitivity to PARP inhibition. This study provides a comprehensive and broadly accessible resource of molecular information for the development of therapeutic avenues in ovarian cancer.
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spelling pubmed-64819452019-04-24 Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines Papp, Eniko Hallberg, Dorothy Konecny, Gottfried E. Bruhm, Daniel C. Adleff, Vilmos Noë, Michaël Kagiampakis, Ioannis Palsgrove, Doreen Conklin, Dylan Kinose, Yasuto White, James R. Press, Michael F. Drapkin, Ronny Easwaran, Hariharan Baylin, Stephen B. Slamon, Dennis Velculescu, Victor E. Scharpf, Robert B. Cell Rep Article To improve our understanding of ovarian cancer, we performed genome-wide analyses of 45 ovarian cancer cell lines. Given the challenges of genomic analyses of tumors without matched normal samples, we developed approaches for detection of somatic sequence and structural changes and integrated these with epigenetic and expression alterations. Alterations not previously implicated in ovarian cancer included amplification or overexpression of ASXL1 and H3F3B, deletion or underexpression of CDC73 and TGF-beta receptor pathway members, and rearrangements of YAP1-MAML2 and IKZF2-ERBB4. Dose-response analyses to targeted therapies revealed unique molecular dependencies, including increased sensitivity of tumors with PIK3CA and PPP2R1A alterations to PI3K inhibitor GNE-493, MYC amplifications to PARP inhibitor BMN673, and SMAD3/4 alterations to MEK inhibitor MEK162. Genome-wide rearrangements provided an improved measure of sensitivity to PARP inhibition. This study provides a comprehensive and broadly accessible resource of molecular information for the development of therapeutic avenues in ovarian cancer. 2018-11-27 /pmc/articles/PMC6481945/ /pubmed/30485824 http://dx.doi.org/10.1016/j.celrep.2018.10.096 Text en This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Papp, Eniko
Hallberg, Dorothy
Konecny, Gottfried E.
Bruhm, Daniel C.
Adleff, Vilmos
Noë, Michaël
Kagiampakis, Ioannis
Palsgrove, Doreen
Conklin, Dylan
Kinose, Yasuto
White, James R.
Press, Michael F.
Drapkin, Ronny
Easwaran, Hariharan
Baylin, Stephen B.
Slamon, Dennis
Velculescu, Victor E.
Scharpf, Robert B.
Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title_full Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title_fullStr Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title_full_unstemmed Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title_short Integrated Genomic, Epigenomic, and Expression Analyses of Ovarian Cancer Cell Lines
title_sort integrated genomic, epigenomic, and expression analyses of ovarian cancer cell lines
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6481945/
https://www.ncbi.nlm.nih.gov/pubmed/30485824
http://dx.doi.org/10.1016/j.celrep.2018.10.096
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