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A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities

Improved efforts are necessary to define the functional product of cancer mutations currently being revealed through large-scale sequencing efforts. Using genome-scale pooled shRNA screening technology, we mapped negative genetic interactions across a set of isogenic cancer cell lines and confirmed...

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Autores principales: Vizeacoumar, Franco J, Arnold, Roland, Vizeacoumar, Frederick S, Chandrashekhar, Megha, Buzina, Alla, Young, Jordan T F, Kwan, Julian H M, Sayad, Azin, Mero, Patricia, Lawo, Steffen, Tanaka, Hiromasa, Brown, Kevin R, Baryshnikova, Anastasia, Mak, Anthony B, Fedyshyn, Yaroslav, Wang, Yadong, Brito, Glauber C, Kasimer, Dahlia, Makhnevych, Taras, Ketela, Troy, Datti, Alessandro, Babu, Mohan, Emili, Andrew, Pelletier, Laurence, Wrana, Jeff, Wainberg, Zev, Kim, Philip M, Rottapel, Robert, O’Brien, Catherine A, Andrews, Brenda, Boone, Charles, Moffat, Jason
Formato: Online Artículo Texto
Lenguaje:English
Publicado: European Molecular Biology Organization 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3817404/
https://www.ncbi.nlm.nih.gov/pubmed/24104479
http://dx.doi.org/10.1038/msb.2013.54
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author Vizeacoumar, Franco J
Arnold, Roland
Vizeacoumar, Frederick S
Chandrashekhar, Megha
Buzina, Alla
Young, Jordan T F
Kwan, Julian H M
Sayad, Azin
Mero, Patricia
Lawo, Steffen
Tanaka, Hiromasa
Brown, Kevin R
Baryshnikova, Anastasia
Mak, Anthony B
Fedyshyn, Yaroslav
Wang, Yadong
Brito, Glauber C
Kasimer, Dahlia
Makhnevych, Taras
Ketela, Troy
Datti, Alessandro
Babu, Mohan
Emili, Andrew
Pelletier, Laurence
Wrana, Jeff
Wainberg, Zev
Kim, Philip M
Rottapel, Robert
O’Brien, Catherine A
Andrews, Brenda
Boone, Charles
Moffat, Jason
author_facet Vizeacoumar, Franco J
Arnold, Roland
Vizeacoumar, Frederick S
Chandrashekhar, Megha
Buzina, Alla
Young, Jordan T F
Kwan, Julian H M
Sayad, Azin
Mero, Patricia
Lawo, Steffen
Tanaka, Hiromasa
Brown, Kevin R
Baryshnikova, Anastasia
Mak, Anthony B
Fedyshyn, Yaroslav
Wang, Yadong
Brito, Glauber C
Kasimer, Dahlia
Makhnevych, Taras
Ketela, Troy
Datti, Alessandro
Babu, Mohan
Emili, Andrew
Pelletier, Laurence
Wrana, Jeff
Wainberg, Zev
Kim, Philip M
Rottapel, Robert
O’Brien, Catherine A
Andrews, Brenda
Boone, Charles
Moffat, Jason
author_sort Vizeacoumar, Franco J
collection PubMed
description Improved efforts are necessary to define the functional product of cancer mutations currently being revealed through large-scale sequencing efforts. Using genome-scale pooled shRNA screening technology, we mapped negative genetic interactions across a set of isogenic cancer cell lines and confirmed hundreds of these interactions in orthogonal co-culture competition assays to generate a high-confidence genetic interaction network of differentially essential or differential essentiality (DiE) genes. The network uncovered examples of conserved genetic interactions, densely connected functional modules derived from comparative genomics with model systems data, functions for uncharacterized genes in the human genome and targetable vulnerabilities. Finally, we demonstrate a general applicability of DiE gene signatures in determining genetic dependencies of other non-isogenic cancer cell lines. For example, the PTEN(−/−) DiE genes reveal a signature that can preferentially classify PTEN-dependent genotypes across a series of non-isogenic cell lines derived from the breast, pancreas and ovarian cancers. Our reference network suggests that many cancer vulnerabilities remain to be discovered through systematic derivation of a network of differentially essential genes in an isogenic cancer cell model.
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spelling pubmed-38174042013-11-06 A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities Vizeacoumar, Franco J Arnold, Roland Vizeacoumar, Frederick S Chandrashekhar, Megha Buzina, Alla Young, Jordan T F Kwan, Julian H M Sayad, Azin Mero, Patricia Lawo, Steffen Tanaka, Hiromasa Brown, Kevin R Baryshnikova, Anastasia Mak, Anthony B Fedyshyn, Yaroslav Wang, Yadong Brito, Glauber C Kasimer, Dahlia Makhnevych, Taras Ketela, Troy Datti, Alessandro Babu, Mohan Emili, Andrew Pelletier, Laurence Wrana, Jeff Wainberg, Zev Kim, Philip M Rottapel, Robert O’Brien, Catherine A Andrews, Brenda Boone, Charles Moffat, Jason Mol Syst Biol Article Improved efforts are necessary to define the functional product of cancer mutations currently being revealed through large-scale sequencing efforts. Using genome-scale pooled shRNA screening technology, we mapped negative genetic interactions across a set of isogenic cancer cell lines and confirmed hundreds of these interactions in orthogonal co-culture competition assays to generate a high-confidence genetic interaction network of differentially essential or differential essentiality (DiE) genes. The network uncovered examples of conserved genetic interactions, densely connected functional modules derived from comparative genomics with model systems data, functions for uncharacterized genes in the human genome and targetable vulnerabilities. Finally, we demonstrate a general applicability of DiE gene signatures in determining genetic dependencies of other non-isogenic cancer cell lines. For example, the PTEN(−/−) DiE genes reveal a signature that can preferentially classify PTEN-dependent genotypes across a series of non-isogenic cell lines derived from the breast, pancreas and ovarian cancers. Our reference network suggests that many cancer vulnerabilities remain to be discovered through systematic derivation of a network of differentially essential genes in an isogenic cancer cell model. European Molecular Biology Organization 2013-10-08 /pmc/articles/PMC3817404/ /pubmed/24104479 http://dx.doi.org/10.1038/msb.2013.54 Text en Copyright © 2013, EMBO and Macmillan Publishers Limited https://creativecommons.org/licenses/by/3.0/This article is licensed under a Creative Commons Attribution 3.0 Unported Licence. To view a copy of this license, visit http://creativecommons.org/licenses/by/3.0/ (https://creativecommons.org/licenses/by/3.0/) .
spellingShingle Article
Vizeacoumar, Franco J
Arnold, Roland
Vizeacoumar, Frederick S
Chandrashekhar, Megha
Buzina, Alla
Young, Jordan T F
Kwan, Julian H M
Sayad, Azin
Mero, Patricia
Lawo, Steffen
Tanaka, Hiromasa
Brown, Kevin R
Baryshnikova, Anastasia
Mak, Anthony B
Fedyshyn, Yaroslav
Wang, Yadong
Brito, Glauber C
Kasimer, Dahlia
Makhnevych, Taras
Ketela, Troy
Datti, Alessandro
Babu, Mohan
Emili, Andrew
Pelletier, Laurence
Wrana, Jeff
Wainberg, Zev
Kim, Philip M
Rottapel, Robert
O’Brien, Catherine A
Andrews, Brenda
Boone, Charles
Moffat, Jason
A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title_full A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title_fullStr A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title_full_unstemmed A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title_short A negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
title_sort negative genetic interaction map in isogenic cancer cell lines reveals cancer cell vulnerabilities
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3817404/
https://www.ncbi.nlm.nih.gov/pubmed/24104479
http://dx.doi.org/10.1038/msb.2013.54
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