Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition

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Recent work has highlighted glutaminase (GLS) as a key player in cancer cell metabolism, providing glutamine-derived carbon and nitrogen to pathways that support proliferation. There is significant interest in targeting GLS for cancer therapy, although the gene is not known to be mutated or amplifie...

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Autores principales: Ulanet, Danielle B., Couto, Kiley, Jha, Abhishek, Choe, Sung, Wang, Amanda, Woo, Hin-Koon, Steadman, Mya, DeLaBarre, Byron, Gross, Stefan, Driggers, Edward, Dorsch, Marion, Hurov, Jonathan B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4264947/
https://www.ncbi.nlm.nih.gov/pubmed/25502225
http://dx.doi.org/10.1371/journal.pone.0115144
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author Ulanet, Danielle B.
Couto, Kiley
Jha, Abhishek
Choe, Sung
Wang, Amanda
Woo, Hin-Koon
Steadman, Mya
DeLaBarre, Byron
Gross, Stefan
Driggers, Edward
Dorsch, Marion
Hurov, Jonathan B.
author_facet Ulanet, Danielle B.
Couto, Kiley
Jha, Abhishek
Choe, Sung
Wang, Amanda
Woo, Hin-Koon
Steadman, Mya
DeLaBarre, Byron
Gross, Stefan
Driggers, Edward
Dorsch, Marion
Hurov, Jonathan B.
author_sort Ulanet, Danielle B.
collection PubMed
description Recent work has highlighted glutaminase (GLS) as a key player in cancer cell metabolism, providing glutamine-derived carbon and nitrogen to pathways that support proliferation. There is significant interest in targeting GLS for cancer therapy, although the gene is not known to be mutated or amplified in tumors. As a result, identification of tractable markers that predict GLS dependence is needed for translation of GLS inhibitors to the clinic. Herein we validate a small molecule inhibitor of GLS and show that non-small cell lung cancer cells marked by low E-cadherin and high vimentin expression, hallmarks of a mesenchymal phenotype, are particularly sensitive to inhibition of the enzyme. Furthermore, lung cancer cells induced to undergo epithelial to mesenchymal transition (EMT) acquire sensitivity to the GLS inhibitor. Metabolic studies suggest that the mesenchymal cells have a reduced capacity for oxidative phosphorylation and increased susceptibility to oxidative stress, rendering them unable to cope with the perturbations induced by GLS inhibition. These findings elucidate selective metabolic dependencies of mesenchymal lung cancer cells and suggest novel pathways as potential targets in this aggressive cancer type.
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spelling pubmed-42649472014-12-19 Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition Ulanet, Danielle B. Couto, Kiley Jha, Abhishek Choe, Sung Wang, Amanda Woo, Hin-Koon Steadman, Mya DeLaBarre, Byron Gross, Stefan Driggers, Edward Dorsch, Marion Hurov, Jonathan B. PLoS One Research Article Recent work has highlighted glutaminase (GLS) as a key player in cancer cell metabolism, providing glutamine-derived carbon and nitrogen to pathways that support proliferation. There is significant interest in targeting GLS for cancer therapy, although the gene is not known to be mutated or amplified in tumors. As a result, identification of tractable markers that predict GLS dependence is needed for translation of GLS inhibitors to the clinic. Herein we validate a small molecule inhibitor of GLS and show that non-small cell lung cancer cells marked by low E-cadherin and high vimentin expression, hallmarks of a mesenchymal phenotype, are particularly sensitive to inhibition of the enzyme. Furthermore, lung cancer cells induced to undergo epithelial to mesenchymal transition (EMT) acquire sensitivity to the GLS inhibitor. Metabolic studies suggest that the mesenchymal cells have a reduced capacity for oxidative phosphorylation and increased susceptibility to oxidative stress, rendering them unable to cope with the perturbations induced by GLS inhibition. These findings elucidate selective metabolic dependencies of mesenchymal lung cancer cells and suggest novel pathways as potential targets in this aggressive cancer type. Public Library of Science 2014-12-12 /pmc/articles/PMC4264947/ /pubmed/25502225 http://dx.doi.org/10.1371/journal.pone.0115144 Text en © 2014 Ulanet 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
Ulanet, Danielle B.
Couto, Kiley
Jha, Abhishek
Choe, Sung
Wang, Amanda
Woo, Hin-Koon
Steadman, Mya
DeLaBarre, Byron
Gross, Stefan
Driggers, Edward
Dorsch, Marion
Hurov, Jonathan B.
Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title_full Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title_fullStr Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title_full_unstemmed Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title_short Mesenchymal Phenotype Predisposes Lung Cancer Cells to Impaired Proliferation and Redox Stress in Response to Glutaminase Inhibition
title_sort mesenchymal phenotype predisposes lung cancer cells to impaired proliferation and redox stress in response to glutaminase inhibition
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4264947/
https://www.ncbi.nlm.nih.gov/pubmed/25502225
http://dx.doi.org/10.1371/journal.pone.0115144
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