GLS2 is protumorigenic in breast cancers

Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, proge...

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Published in	Oncogene Vol. 39; no. 3; pp. 690 - 702
Main Authors	Dias, Marilia M., Adamoski, Douglas, dos Reis, Larissa M., Ascenção, Carolline F. R., de Oliveira, Krishina R. S., Mafra, Ana Carolina Paschoalini, da Silva Bastos, Alliny Cristiny, Quintero, Melissa, de G. Cassago, Carolina, Ferreira, Igor M., Fidelis, Carlos H. V., Rocco, Silvana A., Bajgelman, Marcio Chaim, Stine, Zachary, Berindan-Neagoe, Ioana, Calin, George A., Ambrosio, Andre Luis Berteli, Dias, Sandra Martha Gomes
Format	Journal Article
Language	English
Published	London Nature Publishing Group UK 16.01.2020 Nature Publishing Group
Subjects	13/1 13/31 13/51 13/89 13/95 14/19 14/34 14/63 38/44 38/70 38/77 38/91 42/109 631/67/1347 631/67/322 631/80/83 64/60 Acetanilide Adult Aged Aged, 80 and over Apoptosis Benzeneacetamides - pharmacology Benzeneacetamides - therapeutic use Breast - pathology Breast - surgery Breast cancer Breast Neoplasms - mortality Breast Neoplasms - pathology Breast Neoplasms - therapy Carcinogenesis - pathology Cell adhesion & migration Cell Biology Cell growth Cell Line, Tumor Cell migration Cell proliferation Clinical trials Disease-Free Survival Drug resistance ErbB-2 protein Female Gene Knockdown Techniques Glutaminase Glutaminase - antagonists & inhibitors Glutaminase - metabolism Glutamine Hormones, Sex Human Genetics Humans Internal Medicine Isoforms Lung cancer Lung Neoplasms - secondary Medical prognosis Medicine Medicine & Public Health Mesenchyme Metastases Metastasis Middle Aged Mitochondria Oncology Phenotypes Physiological aspects Progesterone Prognosis Sulfides Sulfides - pharmacology Sulfides - therapeutic use Therapeutic applications Thiadiazoles - pharmacology Thiadiazoles - therapeutic use Tumor suppressor genes Vimentin Romania
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ISSN	0950-9232 1476-5594 1476-5594
DOI	10.1038/s41388-019-1007-z

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Abstract	Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, progesterone, and Her2 receptors) has elevated GLS protein levels and reportedly depends on exogenous glutamine and GLS activity for survival. Despite having high GLS levels, we verified that several breast cancer cells (including TN cells) express endogenous GLS2, defying its role as a bona fide tumor suppressor. Moreover, ectopic GLS2 expression rescued cell proliferation, TCA anaplerosis, redox balance, and mitochondrial function after GLS inhibition by the small molecule currently in clinical trials CB-839 or GLS knockdown of GLS-dependent cell lines. In several cell lines, GLS2 knockdown decreased cell proliferation and glutamine-linked metabolic phenotypes. Strikingly, long-term treatment of TN cells with another GLS-exclusive inhibitor bis-2′-(5-phenylacetamide-1,3,4-thiadiazol-2-yl)ethyl sulfide (BPTES) selected for a drug-resistant population with increased endogenous GLS2 and restored proliferative capacity. GLS2 was linked to enhanced in vitro cell migration and invasion, mesenchymal markers (through the ERK-ZEB1-vimentin axis under certain conditions) and in vivo lung metastasis. Of concern, GLS2 amplification or overexpression is linked to an overall, disease-free and distant metastasis-free worse survival prognosis in breast cancer. Altogether, these data establish an unforeseen role of GLS2 in sustaining tumor proliferation and underlying metastasis in breast cancer and provide an initial framework for exploring GLS2 as a novel therapeutic target.
AbstractList	Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, progesterone, and Her2 receptors) has elevated GLS protein levels and reportedly depends on exogenous glutamine and GLS activity for survival. Despite having high GLS levels, we verified that several breast cancer cells (including TN cells) express endogenous GLS2, defying its role as a bona fide tumor suppressor. Moreover, ectopic GLS2 expression rescued cell proliferation, TCA anaplerosis, redox balance, and mitochondrial function after GLS inhibition by the small molecule currently in clinical trials CB-839 or GLS knockdown of GLS-dependent cell lines. In several cell lines, GLS2 knockdown decreased cell proliferation and glutamine-linked metabolic phenotypes. Strikingly, long-term treatment of TN cells with another GLS-exclusive inhibitor bis-2'-(5-phenylacetamide-1,3,4-thiadiazol-2-yl)ethyl sulfide (BPTES) selected for a drug-resistant population with increased endogenous GLS2 and restored proliferative capacity. GLS2 was linked to enhanced in vitro cell migration and invasion, mesenchymal markers (through the ERK-ZEB1-vimentin axis under certain conditions) and in vivo lung metastasis. Of concern, GLS2 amplification or overexpression is linked to an overall, disease-free and distant metastasis-free worse survival prognosis in breast cancer. Altogether, these data establish an unforeseen role of GLS2 in sustaining tumor proliferation and underlying metastasis in breast cancer and provide an initial framework for exploring GLS2 as a novel therapeutic target.Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, progesterone, and Her2 receptors) has elevated GLS protein levels and reportedly depends on exogenous glutamine and GLS activity for survival. Despite having high GLS levels, we verified that several breast cancer cells (including TN cells) express endogenous GLS2, defying its role as a bona fide tumor suppressor. Moreover, ectopic GLS2 expression rescued cell proliferation, TCA anaplerosis, redox balance, and mitochondrial function after GLS inhibition by the small molecule currently in clinical trials CB-839 or GLS knockdown of GLS-dependent cell lines. In several cell lines, GLS2 knockdown decreased cell proliferation and glutamine-linked metabolic phenotypes. Strikingly, long-term treatment of TN cells with another GLS-exclusive inhibitor bis-2'-(5-phenylacetamide-1,3,4-thiadiazol-2-yl)ethyl sulfide (BPTES) selected for a drug-resistant population with increased endogenous GLS2 and restored proliferative capacity. GLS2 was linked to enhanced in vitro cell migration and invasion, mesenchymal markers (through the ERK-ZEB1-vimentin axis under certain conditions) and in vivo lung metastasis. Of concern, GLS2 amplification or overexpression is linked to an overall, disease-free and distant metastasis-free worse survival prognosis in breast cancer. Altogether, these data establish an unforeseen role of GLS2 in sustaining tumor proliferation and underlying metastasis in breast cancer and provide an initial framework for exploring GLS2 as a novel therapeutic target. Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, progesterone, and Her2 receptors) has elevated GLS protein levels and reportedly depends on exogenous glutamine and GLS activity for survival. Despite having high GLS levels, we verified that several breast cancer cells (including TN cells) express endogenous GLS2, defying its role as a bona fide tumor suppressor. Moreover, ectopic GLS2 expression rescued cell proliferation, TCA anaplerosis, redox balance, and mitochondrial function after GLS inhibition by the small molecule currently in clinical trials CB-839 or GLS knockdown of GLS-dependent cell lines. In several cell lines, GLS2 knockdown decreased cell proliferation and glutamine-linked metabolic phenotypes. Strikingly, long-term treatment of TN cells with another GLS-exclusive inhibitor bis-2'-(5-phenylacetamide-1,3,4-thiadiazol-2-yl)ethyl sulfide (BPTES) selected for a drug-resistant population with increased endogenous GLS2 and restored proliferative capacity. GLS2 was linked to enhanced in vitro cell migration and invasion, mesenchymal markers (through the ERK-ZEB1-vimentin axis under certain conditions) and in vivo lung metastasis. Of concern, GLS2 amplification or overexpression is linked to an overall, disease-free and distant metastasis-free worse survival prognosis in breast cancer. Altogether, these data establish an unforeseen role of GLS2 in sustaining tumor proliferation and underlying metastasis in breast cancer and provide an initial framework for exploring GLS2 as a novel therapeutic target. Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS) isoforms. Conversely, GLS2 variants often have tumor-suppressing activity. Triple-negative (TN) breast cancer (testing negative for estrogen, progesterone, and Her2 receptors) has elevated GLS protein levels and reportedly depends on exogenous glutamine and GLS activity for survival. Despite having high GLS levels, we verified that several breast cancer cells (including TN cells) express endogenous GLS2, defying its role as a bona fide tumor suppressor. Moreover, ectopic GLS2 expression rescued cell proliferation, TCA anaplerosis, redox balance, and mitochondrial function after GLS inhibition by the small molecule currently in clinical trials CB-839 or GLS knockdown of GLS-dependent cell lines. In several cell lines, GLS2 knockdown decreased cell proliferation and glutamine-linked metabolic phenotypes. Strikingly, long-term treatment of TN cells with another GLS-exclusive inhibitor bis-2′-(5-phenylacetamide-1,3,4-thiadiazol-2-yl)ethyl sulfide (BPTES) selected for a drug-resistant population with increased endogenous GLS2 and restored proliferative capacity. GLS2 was linked to enhanced in vitro cell migration and invasion, mesenchymal markers (through the ERK-ZEB1-vimentin axis under certain conditions) and in vivo lung metastasis. Of concern, GLS2 amplification or overexpression is linked to an overall, disease-free and distant metastasis-free worse survival prognosis in breast cancer. Altogether, these data establish an unforeseen role of GLS2 in sustaining tumor proliferation and underlying metastasis in breast cancer and provide an initial framework for exploring GLS2 as a novel therapeutic target.
Audience	Academic
Author	Adamoski, Douglas Ascenção, Carolline F. R. Dias, Marilia M. Rocco, Silvana A. Bajgelman, Marcio Chaim Ferreira, Igor M. Stine, Zachary Berindan-Neagoe, Ioana dos Reis, Larissa M. de G. Cassago, Carolina Dias, Sandra Martha Gomes da Silva Bastos, Alliny Cristiny Fidelis, Carlos H. V. Ambrosio, Andre Luis Berteli Mafra, Ana Carolina Paschoalini de Oliveira, Krishina R. S. Quintero, Melissa Calin, George A.
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Cites_doi	10.1016/j.neuint.2014.11.004 10.1007/BF00666165 10.1016/j.molcel.2010.02.020 10.1172/JCI45014 10.1016/j.cmet.2017.12.006 10.1091/mbc.e07-03-0249 10.1073/pnas.1112495109 10.1073/pnas.1203244109 10.1016/j.ccr.2010.08.009 10.1128/MCB.20.23.8845-8854.2000 10.1152/physiolgenomics.1999.1.2.51 10.18632/oncotarget.6879 10.1038/s41598-017-16327-z 10.1038/emm.2014.99 10.1038/nature07823 10.1158/2159-8290.CD-12-0095 10.1371/journal.pone.0010767 10.1158/1541-7786.MCR-13-0576 10.1016/j.canlet.2016.09.009 10.1038/sj.pcan.4500606 10.18632/oncotarget.5821 10.1371/journal.pone.0038380 10.18632/oncotarget.13116 10.3322/caac.20073 10.18632/oncotarget.2173 10.1371/journal.pone.0185092 10.1073/pnas.1002459107 10.1101/gad.1985910 10.1016/j.cmet.2011.12.015 10.1186/1475-2867-13-76 10.1089/ars.2012.4999 10.1038/nature12040 10.1158/1535-7163.MCT-13-0870 10.1016/j.humpath.2015.05.010 10.4155/fmc-2016-0190 10.18632/oncotarget.13771 10.1158/0008-5472.CAN-10-1666 10.1021/acs.biochem.8b00773 10.4161/cbt.21348 10.1016/j.ajpath.2011.11.030 10.1158/1535-7163.MCT-08-0589 10.18632/oncotarget.3862 10.1073/pnas.1001006107 10.18632/oncotarget.1862 10.1016/j.bbamcr.2006.10.001 10.1016/j.cmet.2013.02.002 10.1083/jcb.201010100 10.1158/1541-7786.MCR-06-0263 10.1016/j.ccr.2013.08.020
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PublicationDate	20200116
PublicationDateYYYYMMDD	2020-01-16
PublicationDate_xml	– month: 1 year: 2020 text: 20200116 day: 16
PublicationDecade	2020
PublicationPlace	London
PublicationPlace_xml	– name: London – name: England – name: New York
PublicationTitle	Oncogene
PublicationTitleAbbrev	Oncogene
PublicationTitleAlternate	Oncogene
PublicationYear	2020
Publisher	Nature Publishing Group UK Nature Publishing Group
Publisher_xml	– name: Nature Publishing Group UK – name: Nature Publishing Group
References	Zhang, Liu, Zhao, Yue, Zhu, Wang (CR20) 2016; 5 Wang, Erickson, Fuji, Ramachandran, Gao, Dinavahi (CR3) 2010; 18 Elgadi, Meguid, Qian, Souba, Abcouwer (CR2) 1999; 1 Kim, Kong, Chang, Kim, Kim (CR40) 2016; 7 Cerami, Gao, Dogrusoz, Gross, Sumer, Aksoy (CR30) 2012; 2 Shirakihara, Saitoh, Miyazono (CR35) 2007; 18 Wellen, Lu, Mancuso, Lemons, Ryczko, Dennis (CR44) 2010; 24 Kuo, Chen, Hua, Yu, Lee (CR21) 2016; 383 Sircar, Huang, Hu, Cogdell, Dhillon, Tzelepi (CR28) 2012; 180 Pavlova, Hui, Ghergurovich, Fan, Intlekofer, White (CR46) 2018; 27 Kung, Marks, Chi (CR12) 2011; 7 Hu, Zhang, Wu, Sun, Levine, Feng (CR14) 2010; 107 Gameiro, Yang, Metelo, Pérez-Carro, Baker, Wang (CR9) 2013; 17 Gross, Demo, Dennison, Chen, Chernov-Rogan, Goyal (CR13) 2014; 13 Liu, Le, Hancock, Lane, Dang, Fan (CR5) 2012; 109 Sánchez-Tilló, Siles, de Barrios, Cuatrecasas, Vaquero, Castells (CR41) 2011; 1 Sommers, Byers, Thompson, Torri, Gelmann (CR37) 1994; 31 Jang, Kim, Kim, Chung, Park (CR34) 2015; 46 CR49 Yuneva, Fan, Allen, Higashi, Ferraris, Tsukamoto (CR7) 2012; 15 Shin, Dimitri, Yoon, Dowdle, Blenis (CR33) 2010; 38 Lee, Jeon, Ju, Jeong, Kim, Park (CR19) 2016; 7 Xu, Takeshita, Hino, Fukunaga, Kudo, Tamaki (CR53) 2011; 193 Suzuki, Tanaka, Poyurovsky, Nagano, Mayama, Ohkubo (CR15) 2010; 107 Katt, Lukey, Cerione (CR29) 2017; 9 Son, Lyssiotis, Ying, Wang, Hua, Ligorio (CR8) 2013; 496 Ubuka, Meister (CR25) 1971; 46 Martín-Rufián, Tosina, Campos-Sandoval, Manzanares, Lobo, Segura, Alonso, Matés, Márquez (CR16) 2012; 7 Nitta, Kozono, Kennedy, Stommel, Ng, Zinn (CR48) 2010; 5 Hollestelle, Elstrodt, Nagel, Kallemeijn, Schutte (CR36) 2007; 5 Gao, Tchernyshyov, Chang, Lee, Kita, Ochi (CR1) 2009; 458 Koh, Koh, Ng, Toh, Sandanaraj, Chong (CR47) 2013; 19 Liu, Zhang, Lin, Zhu, Liang, Hong (CR18) 2014; 5 Lehmann, Bauer, Chen, Sanders, Chakravarthy, Shyr (CR23) 2011; 121 Xiao, Ren, Su, Yue, Xiu, Hu (CR22) 2015; 6 Xu, Zhang, Ishida, Hajjar, Tang, Shi (CR39) 2016; 8 Cassago, Ferreira, Ferreira, Fornezari, Gomes, Greene (CR11) 2012; 109 Szeliga, Albrecht (CR17) 2015; 88 Lorenzi, Llamas, Gunsior, Ozbun, Reinhold, Varma (CR26) 2008; 7 Seltzer, Bennett, Joshi, Gao, Thomas, Ferraris (CR4) 2010; 70 Bastide, Bagnis, Mannoni, Hassoun, Bladou (CR50) 2002; 5 Panosyan, Wang, Xia, Lee, Pak, Laks (CR27) 2014; 12 McCubrey, Steelman, Chappell, Abrams, Wong, Chang (CR42) 2007; 1773 Lampa, Arlt, He, Ospina, Reeves, Zhang, Murtie, Deng, Barberis, Hoffmann, Cheng, Pollard, Winter, Richon, Garcia-Escheverria, Adrian, Wiederschain, Srinivasan (CR24) 2017; 12 Lee, Yang, Chang, Hsu, Qiu, Chao (CR52) 2014; 5 van den Heuvel, Jing, Wooster, Bachman (CR6) 2012; 13 Billin, Eilers, Coulter, Logan, Ayer (CR45) 2000; 20 Timmerman, Holton, Yuneva, Louie, Padró, Daemen (CR10) 2013; 24 Davis, Parsonage, Cabot, Parat, Thompson (CR38) 2013; 13 Zacharias, McCullough, Shanmugavelandy, Lee, Lee, Dutta (CR43) 2017; 7 Kim, Suh, Yoo, Cui, Kim, Kim (CR51) 2015; 47 Jemal, Siegel, Xu, Ward (CR31) 2010; 60 Liu, Lin, Tang, Wang (CR32) 2015; 6 PA Gameiro (1007_CR9) 2013; 17 W Hu (1007_CR14) 2010; 107 T Shirakihara (1007_CR35) 2007; 18 MO Yuneva (1007_CR7) 2012; 15 A Cassago (1007_CR11) 2012; 109 Michael Lampa (1007_CR24) 2017; 12 T Ubuka (1007_CR25) 1971; 46 S Suzuki (1007_CR15) 2010; 107 PL Lorenzi (1007_CR26) 2008; 7 Y-Z Lee (1007_CR52) 2014; 5 D Xu (1007_CR53) 2011; 193 HN Kung (1007_CR12) 2011; 7 LW-H Koh (1007_CR47) 2013; 19 MH Jang (1007_CR34) 2015; 46 EH Panosyan (1007_CR27) 2014; 12 C Bastide (1007_CR50) 2002; 5 NN Pavlova (1007_CR46) 2018; 27 J Son (1007_CR8) 2013; 496 J Kim (1007_CR40) 2016; 7 M Nitta (1007_CR48) 2010; 5 S Shin (1007_CR33) 2010; 38 RK Kim (1007_CR51) 2015; 47 A Hollestelle (1007_CR36) 2007; 5 CL Sommers (1007_CR37) 1994; 31 JA McCubrey (1007_CR42) 2007; 1773 APJ van den Heuvel (1007_CR6) 2012; 13 MI Gross (1007_CR13) 2014; 13 LA Timmerman (1007_CR10) 2013; 24 M Szeliga (1007_CR17) 2015; 88 W Liu (1007_CR5) 2012; 109 C Zhang (1007_CR20) 2016; 5 Mercedes Martín-Rufián (1007_CR16) 2012; 7 D Xiao (1007_CR22) 2015; 6 MJ Seltzer (1007_CR4) 2010; 70 A Jemal (1007_CR31) 2010; 60 Q Xu (1007_CR39) 2016; 8 T Kuo (1007_CR21) 2016; 383 aN Billin (1007_CR45) 2000; 20 KM Elgadi (1007_CR2) 1999; 1 E Cerami (1007_CR30) 2012; 2 J-BBin Wang (1007_CR3) 2010; 18 J Liu (1007_CR18) 2014; 5 SY Lee (1007_CR19) 2016; 7 P Gao (1007_CR1) 2009; 458 NM Zacharias (1007_CR43) 2017; 7 1007_CR49 E Sánchez-Tilló (1007_CR41) 2011; 1 WP Katt (1007_CR29) 2017; 9 KE Wellen (1007_CR44) 2010; 24 C-Y Liu (1007_CR32) 2015; 6 K Sircar (1007_CR28) 2012; 180 FM Davis (1007_CR38) 2013; 13 BD Lehmann (1007_CR23) 2011; 121
References_xml	– volume: 31 start-page: 325 year: 1994 end-page: 35 ident: CR37 article-title: Differentiation state and invasiveness of human breast cancer cell lines publication-title: Breast Cancer Res Treat – volume: 5 start-page: 195 year: 2007 end-page: 201 ident: CR36 article-title: Phosphatidylinositol-3-OH Kinase or RAS Pathway Mutations in Human Breast Cancer Cell Lines publication-title: Mol Cancer Res – ident: CR49 – volume: 1 start-page: 51 year: 1999 end-page: 62 ident: CR2 article-title: Cloning and analysis of unique human glutaminase isoforms generated by tissue-specific alternative splicing publication-title: Physiol Genom – volume: 9 start-page: 223 year: 2017 end-page: 43 ident: CR29 article-title: A tale of two glutaminases: homologous enzymes with distinct roles in tumorigenesis publication-title: Future Med Chem – volume: 70 start-page: 8981 year: 2010 end-page: 7 ident: CR4 article-title: Inhibition of glutaminase preferentially slows growth of glioma cells with mutant IDH1 publication-title: Cancer Res – volume: 6 start-page: 40655 year: 2015 end-page: 66 ident: CR22 article-title: Myc promotes glutaminolysis in human neuroblastoma through direct activation of glutaminase 2 publication-title: Oncotarget – volume: 1 start-page: 897 year: 2011 end-page: 912 ident: CR41 article-title: Expanding roles of ZEB factors in tumorigenesis and tumor progression publication-title: Am J Cancer Res – volume: 193 start-page: 409 year: 2011 end-page: 24 ident: CR53 article-title: miR-22 represses cancer progression by inducing cellular senescence publication-title: J Cell Biol – volume: 6 start-page: 15966 year: 2015 end-page: 83 ident: CR32 article-title: Vimentin contributes to epithelial-mesenchymal transition cancer cell mechanics by mediating cytoskeletal organization and focal adhesion maturation publication-title: Oncotarget – volume: 13 year: 2013 ident: CR38 article-title: Assessment of gene expression of intracellular calcium channels, pumps and exchangers with epidermal growth factor-induced epithelial-mesenchymal transition in a breast cancer cell line publication-title: Cancer Cell Int – volume: 180 start-page: 895 year: 2012 end-page: 903 ident: CR28 article-title: Integrative molecular profiling reveals asparagine synthetase is a target in castration-resistant prostate cancer publication-title: Am J Pathol – volume: 18 start-page: 207 year: 2010 end-page: 19 ident: CR3 article-title: Targeting mitochondrial glutaminase activity inhibits oncogenic transformation publication-title: Cancer Cell – volume: 107 start-page: 7461 year: 2010 end-page: 6 ident: CR15 article-title: Phosphate-activated glutaminase (GLS2), a p53-inducible regulator of glutamine metabolism and reactive oxygen species publication-title: Proc Natl Acad Sci USA – volume: 121 start-page: 2750 year: 2011 end-page: 67 ident: CR23 article-title: Identification of human triple-negative breast cancer subtypes and preclinical models for selection of targeted therapies publication-title: J Clin Investig – volume: 7 start-page: e38380 issue: 6 year: 2012 ident: CR16 article-title: Mammalian Glutaminase Gls2 Gene Encodes Two Functional Alternative Transcripts by a Surrogate Promoter Usage Mechanism publication-title: PLoS ONE – volume: 2 start-page: 401 year: 2012 end-page: 4 ident: CR30 article-title: The cBio cancer genomics portal: an open platform for exploring multidimensional cancer genomics data publication-title: Cancer Discov – volume: 7 start-page: 7925 year: 2016 end-page: 39 ident: CR19 article-title: Dlx-2 and glutaminase upregulate epithelial-mesenchymal transition and glycolytic switch publication-title: Oncotarget – volume: 7 start-page: 3123 year: 2008 end-page: 8 ident: CR26 article-title: Asparagine synthetase is a predictive biomarker of L-asparaginase activity in ovarian cancer cell lines publication-title: Mol Cancer Ther – volume: 24 start-page: 450 year: 2013 end-page: 65 ident: CR10 article-title: Glutamine sensitivity analysis identifies the xCT antiporter as a common triple-negative breast tumor therapeutic target publication-title: Cancer Cell – volume: 7 year: 2011 ident: CR12 article-title: Glutamine synthetase is a genetic determinant of cell type-specific glutamine independence in breast epithelia publication-title: PLoS Genet – volume: 13 start-page: 1185 year: 2012 end-page: 94 ident: CR6 article-title: Analysis of glutamine dependency in non-small cell lung cancer publication-title: Cancer Biol Ther – volume: 15 start-page: 157 year: 2012 end-page: 70 ident: CR7 article-title: The metabolic profile of tumors depends on both the responsible genetic lesion and tissue type publication-title: Cell Metab – volume: 13 start-page: 890 year: 2014 end-page: 901 ident: CR13 article-title: Antitumor activity of the glutaminase inhibitor CB-839 in triple-negative breast cancer publication-title: Mol Cancer Ther – volume: 47 start-page: e137 year: 2015 end-page: 9 ident: CR51 article-title: Activation of KRAS promotes the mesenchymal features of basal-type breast cancer publication-title: Exp Mol Med – volume: 27 start-page: 428 year: 2018 end-page: 38 ident: CR46 article-title: As extracellular glutamine levels decline, asparagine becomes an essential amino acid publication-title: Cell Metab. – volume: 19 start-page: 2261 year: 2013 end-page: 79 ident: CR47 article-title: A distinct reactive oxygen species profile confers chemoresistance in glioma-propagating cells and associates with patient survival outcome publication-title: Antioxid Redox Signal – volume: 5 start-page: 311 year: 2002 end-page: 5 ident: CR50 article-title: A Nod Scid mouse model to study human prostate cancer publication-title: Prostate Cancer Prostatic Dis – volume: 88 start-page: 6 year: 2015 end-page: 9 ident: CR17 article-title: Opposing roles of glutaminase isoforms in determining glioblastoma cell phenotype publication-title: Neurochem Int – volume: 8 start-page: 9557 year: 2016 end-page: 71 ident: CR39 article-title: EGF induces epithelial-mesenchymal transition and cancer stem-like cell properties in human oral cancer cells via promoting warburg effect publication-title: Oncotarget – volume: 458 start-page: 762 year: 2009 end-page: 5 ident: CR1 article-title: c-Myc suppression of miR-23a/b enhances mitochondrial glutaminase expression and glutamine metabolism publication-title: Nature – volume: 496 start-page: 101 year: 2013 end-page: 5 ident: CR8 article-title: Glutamine supports pancreatic cancer growth through a KRAS-regulated metabolic pathway publication-title: Nature – volume: 1773 start-page: 1263 year: 2007 end-page: 84 ident: CR42 article-title: Roles of the Raf/MEK/ERK pathway in cell growth, malignant transformation and drug resistance publication-title: Biochim Biophys Acta – volume: 17 start-page: 372 year: 2013 end-page: 85 ident: CR9 article-title: In vivo HIF-mediated reductive carboxylation is regulated by citrate levels and sensitizes VHL-deficient cells to glutamine deprivation publication-title: Cell Metab – volume: 18 start-page: 3533 year: 2007 end-page: 44 ident: CR35 article-title: Differential regulation of epithelial and mesenchymal markers by δEF1 proteins in epithelial–mesenchymal transition induced by TGF-β publication-title: Mol Biol Cell – volume: 107 start-page: 7455 year: 2010 end-page: 60 ident: CR14 article-title: Glutaminase 2, a novel p53 target gene regulating energy metabolism and antioxidant function publication-title: Proc Natl Acad Sci USA – volume: 46 start-page: 291 year: 1971 end-page: 8 ident: CR25 article-title: Studies on the utilization of asparagine by mouse leukemia cells publication-title: J Natl Cancer Inst – volume: 109 start-page: 8983 year: 2012 end-page: 8 ident: CR5 article-title: Reprogramming of proline and glutamine metabolism contributes to the proliferative and metabolic responses regulated by oncogenic transcription factor c-MYC publication-title: Proc Natl Acad Sci USA – volume: 60 start-page: 277 year: 2010 end-page: 300 ident: CR31 article-title: Cancer statistics, 2010 publication-title: CA Cancer J Clin – volume: 7 start-page: 85021 year: 2016 end-page: 32 ident: CR40 article-title: EGF induces epithelial-mesenchymal transition through phospho-Smad2/3-Snail signaling pathway in breast cancer cells publication-title: Oncotarget – volume: 109 start-page: 1092 year: 2012 end-page: 7 ident: CR11 article-title: Mitochondrial localization and structure-based phosphate activation mechanism of Glutaminase C with implications for cancer metabolism publication-title: Proc Natl Acad Sci – volume: 7 start-page: 1 year: 2017 end-page: 11 ident: CR43 article-title: Metabolic differences in glutamine utilization lead to metabolic vulnerabilities in prostate cancer publication-title: Sci Rep – volume: 5 start-page: 1 year: 2016 end-page: 20 ident: CR20 article-title: Glutaminase 2 is a novel negative regulator of small GTPase Rac1 and mediates p53 function in suppressing metastasis publication-title: Elife – volume: 5 start-page: 6087 year: 2014 end-page: 101 ident: CR52 article-title: Discovery of selective inhibitors of Glutaminase-2, which inhibit mTORC1, activate autophagy and inhibit proliferation in cancer cells publication-title: Oncotarget – volume: 38 start-page: 114 year: 2010 end-page: 27 ident: CR33 article-title: ERK2 but not ERK1, induces epithelial to mesenchymal transformation via DEF motif dependent signaling events publication-title: Mol Cell – volume: 24 start-page: 2784 year: 2010 end-page: 99 ident: CR44 article-title: The hexosamine biosynthetic pathway couples growth factor-induced glutamine uptake to glucose metabolism publication-title: Genes Dev – volume: 12 start-page: e0185092 issue: 9 year: 2017 ident: CR24 article-title: Glutaminase is essential for the growth of triple-negative breast cancer cells with a deregulated glutamine metabolism pathway and its suppression synergizes with mTOR inhibition publication-title: PLOS ONE – volume: 383 start-page: 1 year: 2016 end-page: 13 ident: CR21 article-title: Glutaminase 2 stabilizes Dicer to repress Snail and metastasis in hepatocellular carcinoma cells publication-title: Cancer Lett – volume: 20 start-page: 8845 year: 2000 end-page: 54 ident: CR45 article-title: MondoA, a novel basic helix-loop-helix-leucine zipper transcriptional activator that constitutes a positive branch of a max-like network publication-title: Mol Cell Biol – volume: 46 start-page: 1267 year: 2015 end-page: 74 ident: CR34 article-title: Expression of epithelial-mesenchymal transition–related markers in triple-negative breast cancer: ZEB1 as a potential biomarker for poor clinical outcome publication-title: Hum Pathol – volume: 5 start-page: 1 year: 2010 end-page: 9 ident: CR48 article-title: Targeting EGFR induced oxidative stress by PARP1 inhibition in glioblastoma therapy publication-title: PLoS ONE – volume: 12 start-page: 694 year: 2014 end-page: 702 ident: CR27 article-title: Asparagine depletion potentiates the cytotoxic effect of chemotherapy against brain tumors publication-title: Mol Cancer Res – volume: 5 start-page: 2635 year: 2014 end-page: 47 ident: CR18 article-title: Glutaminase 2 negatively regulates the PI3K / AKT signaling and shows tumor suppression activity in human hepatocellular carcinoma publication-title: Oncotarget – volume: 88 start-page: 6 year: 2015 ident: 1007_CR17 publication-title: Neurochem Int doi: 10.1016/j.neuint.2014.11.004 – volume: 31 start-page: 325 year: 1994 ident: 1007_CR37 publication-title: Breast Cancer Res Treat doi: 10.1007/BF00666165 – volume: 38 start-page: 114 year: 2010 ident: 1007_CR33 publication-title: Mol Cell doi: 10.1016/j.molcel.2010.02.020 – volume: 121 start-page: 2750 year: 2011 ident: 1007_CR23 publication-title: J Clin Investig doi: 10.1172/JCI45014 – volume: 27 start-page: 428 year: 2018 ident: 1007_CR46 publication-title: Cell Metab. doi: 10.1016/j.cmet.2017.12.006 – volume: 18 start-page: 3533 year: 2007 ident: 1007_CR35 publication-title: Mol Biol Cell doi: 10.1091/mbc.e07-03-0249 – volume: 109 start-page: 1092 year: 2012 ident: 1007_CR11 publication-title: Proc Natl Acad Sci doi: 10.1073/pnas.1112495109 – volume: 109 start-page: 8983 year: 2012 ident: 1007_CR5 publication-title: Proc Natl Acad Sci USA doi: 10.1073/pnas.1203244109 – volume: 18 start-page: 207 year: 2010 ident: 1007_CR3 publication-title: Cancer Cell doi: 10.1016/j.ccr.2010.08.009 – volume: 20 start-page: 8845 year: 2000 ident: 1007_CR45 publication-title: Mol Cell Biol doi: 10.1128/MCB.20.23.8845-8854.2000 – volume: 1 start-page: 51 year: 1999 ident: 1007_CR2 publication-title: Physiol Genom doi: 10.1152/physiolgenomics.1999.1.2.51 – volume: 7 start-page: 7925 year: 2016 ident: 1007_CR19 publication-title: Oncotarget doi: 10.18632/oncotarget.6879 – volume: 7 start-page: 1 year: 2017 ident: 1007_CR43 publication-title: Sci Rep doi: 10.1038/s41598-017-16327-z – volume: 46 start-page: 291 year: 1971 ident: 1007_CR25 publication-title: J Natl Cancer Inst – volume: 47 start-page: e137 year: 2015 ident: 1007_CR51 publication-title: Exp Mol Med doi: 10.1038/emm.2014.99 – volume: 458 start-page: 762 year: 2009 ident: 1007_CR1 publication-title: Nature doi: 10.1038/nature07823 – volume: 5 start-page: 1 year: 2016 ident: 1007_CR20 publication-title: Elife – volume: 2 start-page: 401 year: 2012 ident: 1007_CR30 publication-title: Cancer Discov doi: 10.1158/2159-8290.CD-12-0095 – volume: 5 start-page: 1 year: 2010 ident: 1007_CR48 publication-title: PLoS ONE doi: 10.1371/journal.pone.0010767 – volume: 12 start-page: 694 year: 2014 ident: 1007_CR27 publication-title: Mol Cancer Res doi: 10.1158/1541-7786.MCR-13-0576 – volume: 383 start-page: 1 year: 2016 ident: 1007_CR21 publication-title: Cancer Lett doi: 10.1016/j.canlet.2016.09.009 – volume: 5 start-page: 311 year: 2002 ident: 1007_CR50 publication-title: Prostate Cancer Prostatic Dis doi: 10.1038/sj.pcan.4500606 – volume: 6 start-page: 40655 year: 2015 ident: 1007_CR22 publication-title: Oncotarget doi: 10.18632/oncotarget.5821 – volume: 7 start-page: e38380 issue: 6 year: 2012 ident: 1007_CR16 publication-title: PLoS ONE doi: 10.1371/journal.pone.0038380 – volume: 7 start-page: 85021 year: 2016 ident: 1007_CR40 publication-title: Oncotarget doi: 10.18632/oncotarget.13116 – volume: 60 start-page: 277 year: 2010 ident: 1007_CR31 publication-title: CA Cancer J Clin doi: 10.3322/caac.20073 – volume: 5 start-page: 6087 year: 2014 ident: 1007_CR52 publication-title: Oncotarget doi: 10.18632/oncotarget.2173 – volume: 12 start-page: e0185092 issue: 9 year: 2017 ident: 1007_CR24 publication-title: PLOS ONE doi: 10.1371/journal.pone.0185092 – volume: 107 start-page: 7461 year: 2010 ident: 1007_CR15 publication-title: Proc Natl Acad Sci USA doi: 10.1073/pnas.1002459107 – volume: 24 start-page: 2784 year: 2010 ident: 1007_CR44 publication-title: Genes Dev doi: 10.1101/gad.1985910 – volume: 15 start-page: 157 year: 2012 ident: 1007_CR7 publication-title: Cell Metab doi: 10.1016/j.cmet.2011.12.015 – volume: 13 year: 2013 ident: 1007_CR38 publication-title: Cancer Cell Int doi: 10.1186/1475-2867-13-76 – volume: 19 start-page: 2261 year: 2013 ident: 1007_CR47 publication-title: Antioxid Redox Signal doi: 10.1089/ars.2012.4999 – volume: 496 start-page: 101 year: 2013 ident: 1007_CR8 publication-title: Nature doi: 10.1038/nature12040 – volume: 13 start-page: 890 year: 2014 ident: 1007_CR13 publication-title: Mol Cancer Ther doi: 10.1158/1535-7163.MCT-13-0870 – volume: 46 start-page: 1267 year: 2015 ident: 1007_CR34 publication-title: Hum Pathol doi: 10.1016/j.humpath.2015.05.010 – volume: 9 start-page: 223 year: 2017 ident: 1007_CR29 publication-title: Future Med Chem doi: 10.4155/fmc-2016-0190 – volume: 8 start-page: 9557 year: 2016 ident: 1007_CR39 publication-title: Oncotarget doi: 10.18632/oncotarget.13771 – volume: 70 start-page: 8981 year: 2010 ident: 1007_CR4 publication-title: Cancer Res doi: 10.1158/0008-5472.CAN-10-1666 – ident: 1007_CR49 doi: 10.1021/acs.biochem.8b00773 – volume: 13 start-page: 1185 year: 2012 ident: 1007_CR6 publication-title: Cancer Biol Ther doi: 10.4161/cbt.21348 – volume: 7 year: 2011 ident: 1007_CR12 publication-title: PLoS Genet – volume: 180 start-page: 895 year: 2012 ident: 1007_CR28 publication-title: Am J Pathol doi: 10.1016/j.ajpath.2011.11.030 – volume: 1 start-page: 897 year: 2011 ident: 1007_CR41 publication-title: Am J Cancer Res – volume: 7 start-page: 3123 year: 2008 ident: 1007_CR26 publication-title: Mol Cancer Ther doi: 10.1158/1535-7163.MCT-08-0589 – volume: 6 start-page: 15966 year: 2015 ident: 1007_CR32 publication-title: Oncotarget doi: 10.18632/oncotarget.3862 – volume: 107 start-page: 7455 year: 2010 ident: 1007_CR14 publication-title: Proc Natl Acad Sci USA doi: 10.1073/pnas.1001006107 – volume: 5 start-page: 2635 year: 2014 ident: 1007_CR18 publication-title: Oncotarget doi: 10.18632/oncotarget.1862 – volume: 1773 start-page: 1263 year: 2007 ident: 1007_CR42 publication-title: Biochim Biophys Acta doi: 10.1016/j.bbamcr.2006.10.001 – volume: 17 start-page: 372 year: 2013 ident: 1007_CR9 publication-title: Cell Metab doi: 10.1016/j.cmet.2013.02.002 – volume: 193 start-page: 409 year: 2011 ident: 1007_CR53 publication-title: J Cell Biol doi: 10.1083/jcb.201010100 – volume: 5 start-page: 195 year: 2007 ident: 1007_CR36 publication-title: Mol Cancer Res doi: 10.1158/1541-7786.MCR-06-0263 – volume: 24 start-page: 450 year: 2013 ident: 1007_CR10 publication-title: Cancer Cell doi: 10.1016/j.ccr.2013.08.020
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Snippet	Many types of cancers have a well-established dependence on glutamine metabolism to support survival and growth, a process linked to glutaminase 1 (GLS)...
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Title	GLS2 is protumorigenic in breast cancers
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