Reprogrammed transsulfuration promotes basal-like breast tumor progression via realigning cellular cysteine persulfidation

被引:57
作者
Erdelyi, Katalin [1 ]
Ditroi, Tamas [1 ]
Johansson, Henrik J. [2 ]
Czikora, Agnes [1 ]
Balog, Noemi [1 ]
Silwal-Pandit, Laxmi [3 ]
Ida, Tomoaki [4 ]
Olasz, Judit [5 ]
Hajdu, Dorottya [1 ]
Matrai, Zoltan [6 ]
Csuka, Orsolya [5 ]
Uchida, Koji [7 ]
Tovari, Jozsef [8 ]
Engebraten, Olav [9 ]
Akaike, Takaaki [4 ]
Dale, Anne-Lise Borresen [3 ]
Kasler, Miklos [10 ]
Lehtio, Janne [2 ]
Nagy, Peter [1 ,11 ,12 ]
机构
[1] Natl Inst Oncol, Dept Mol Immunol & Toxicol, H-1122 Budapest, Hungary
[2] Karolinska Inst, Dept Oncol Pathol, Sci Life Lab, S-17121 Solna, Sweden
[3] Oslo Univ Hosp, Inst Canc Res, Dept Canc Genet, N-0379 Oslo, Norway
[4] Tohoku Univ, Dept Environm Med & Mol Toxicol, Grad Sch Med, Sendai, Miyagi 9808575, Japan
[5] Natl Inst Oncol, Dept Pathogenet, H-1122 Budapest, Hungary
[6] Natl Inst Oncol, Dept Surg, H-1122 Budapest, Hungary
[7] Univ Tokyo, Grad Sch Agr & Life Sci, Dept Appl Biol Chem, Tokyo 113, Japan
[8] Natl Inst Oncol, Dept Expt Pharmacol, H-1122 Budapest, Hungary
[9] Univ Oslo, Oslo Univ Hosp, Fac Med, Inst Canc Res, N-0372 Oslo, Norway
[10] Natl Inst Oncol, Dept Head & Neck Surg, H-1122 Budapest, Hungary
[11] Univ Vet Med, Dept Anat & Histol, H-1078 Budapest, Hungary
[12] Univ Debrecen, Inst Oncochem, H-4012 Debrecen, Hungary
基金
日本学术振兴会; 瑞典研究理事会; 欧盟地平线“2020”;
关键词
persulfide; transsulfuration; hydrogen sulfide; basal-like breast cancer; cystathione beta-synthetase; CYSTATHIONINE-BETA-SYNTHASE; HYDROGEN-SULFIDE; OXIDATIVE STRESS; PROLIFERATION; ANGIOGENESIS; METABOLISM; MECHANISMS; HYPOXIA; BIOLOGY; H2O2;
D O I
10.1073/pnas.2100050118
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Basal like breast cancer (BLBC) is the most aggressive subtype of breast tumors with poor prognosis and limited molecular targeted therapy options. We show that BLBC cells have a high Cys demand and reprogrammed Cys metabolism. Patient-derived BLBC tumors from four different cohorts exhibited elevated expression of the transsulfuration enzyme cystathione beta-synthetase (CBS). CBS silencing (shCBS) made BLBC cells less invasive, proliferate slower, more vulnerable to oxidative stress and cystine (CySSCy) deprivation, prone to ferroptosis, and less responsive to HIF1-alpha activation under hypoxia. shCBS xenograft tumors grew slower than controls and exhibited impaired angiogenesis and larger necrotic areas. Sulfur metabolite profiling suggested that realigned sulfide/persulfide-inducing functions of CBS are important in BLBC tumor progression. Supporting this, the exclusion of serine, a substrate of CBS for producing Cys but not for producing sulfide/persulfide, did not exacerbate CySSCy deprivation-induced ferroptosis in shCBS BLBC cells. Impaired Tyr phosphorylation was detected in shCBS cells and xenografts, likely due to persulfidation-inhibited phosphatase functions. Overexpression of cystathione gamma-lyase (CSE), which can also contribute to cellular sulfide/persulfide production, compensated for the loss of CBS activities, and treatment of shCBS xenografts with a CSE inhibitor further blocked tumor growth. Glutathione and protein-Cys levels were not diminished in shCBS cells or xenografts, but levels of Cys persulfidation and the persulfide-catabolizing enzyme ETHE1 were suppressed. Finally, expression of enzymes of the oxidizing Cys catabolism pathway was diminished, but expression of the persulfide-producing CARS2 was elevated in human BLBC tumors. Hence, the persulfide-producing pathways are major targetable determinants of BLBC pathology that could be therapeutically exploited.
引用
收藏
页数:12
相关论文
共 60 条
[1]   Cysteinyl-tRNA synthetase governs cysteine polysulfidation and mitochondrial bioenergetics [J].
Akaike, Takaaki ;
Ida, Tomoaki ;
Wei, Fan-Yan ;
Nishida, Motohiro ;
Kumagai, Yoshito ;
Alam, Md. Morshedul ;
Ihara, Hideshi ;
Sawa, Tomohiro ;
Matsunaga, Tetsuro ;
Kasamatsu, Shingo ;
Nishimura, Akiyuki ;
Morita, Masanobu ;
Tomizawa, Kazuhito ;
Nishimura, Akira ;
Watanabe, Satoshi ;
Inaba, Kenji ;
Shima, Hiroshi ;
Tanuma, Nobuhiro ;
Jung, Minkyung ;
Fujii, Shigemoto ;
Watanabe, Yasuo ;
Ohmuraya, Masaki ;
Nagy, Peter ;
Feelisch, Martin ;
Fukuto, Jon M. ;
Motohashi, Hozumi .
NATURE COMMUNICATIONS, 2017, 8
[2]   Integrative clustering reveals a novel split in the luminal A subtype of breast cancer with impact on outcome [J].
Aure, Miriam Ragle ;
Vitelli, Valeria ;
Jernstrom, Sandra ;
Kumar, Surendra ;
Krohn, Marit ;
Due, Eldri U. ;
Haukaas, Tonje Husby ;
Leivonen, Suvi-Katri ;
Vollan, Hans Kristian Moen ;
Luders, Torben ;
Rodland, Einar ;
Vaske, Charles J. ;
Zhao, Wei ;
Moller, Elen K. ;
Nord, Silje ;
Giskeodegard, Guro F. ;
Bathen, Tone Frost ;
Caldas, Carlos ;
Tramm, Trine ;
Alsner, Jan ;
Overgaard, Jens ;
Geisler, Jurgen ;
Bukholm, Ida R. K. ;
Naume, Bjorn ;
Schlichting, Ellen ;
Sauer, Torill ;
Mills, Gordon B. ;
Karesen, Rolf ;
Maelandsmo, Gunhild M. ;
Lingjaerde, Ole Christian ;
Frigessi, Arnoldo ;
Kristensen, Vessela N. ;
Borresen-Dale, Anne-Lise ;
Sahlberg, Kristine K. .
BREAST CANCER RESEARCH, 2017, 19
[3]   Integrated analysis reveals microRNA networks coordinately expressed with key proteins in breast cancer [J].
Aure, Miriam Ragle ;
Jernstrom, Sandra ;
Krohn, Marit ;
Vollan, Hans Kristian Moen ;
Due, Eldri U. ;
Rodland, Einar ;
Karesen, Rolf ;
Ram, Prahlad ;
Lu, Yiling ;
Mills, Gordon B. ;
Sahlberg, Kristine Kleivi ;
Borresen-Dale, Anne-Lise ;
Lingjaerde, Ole Christian ;
Kristensen, Vessela N. .
GENOME MEDICINE, 2015, 7
[4]   Speciation of reactive sulfur species and their reactions with alkylating agents: do we have any clue about what is present inside the cell? [J].
Bogdandi, Virag ;
Ida, Tomoaki ;
Sutton, Thomas R. ;
Bianco, Christopher ;
Ditroi, Tamas ;
Koster, Grielof ;
Henthorn, Hillary A. ;
Minnion, Magda ;
Toscano, John P. ;
van der Vliet, Albert ;
Pluth, Michael D. ;
Feelisch, Martin ;
Fukuto, Jon M. ;
Akaike, Takaaki ;
Nagy, Peter .
BRITISH JOURNAL OF PHARMACOLOGY, 2019, 176 (04) :646-670
[5]   The Soft Agar Colony Formation Assay [J].
Borowicz, Stanley ;
Van Scoyk, Michelle ;
Avasarala, Sreedevi ;
Rathinam, Manoj Kumar Karuppusamy ;
Tauler, Jordi ;
Bikkavilli, Rama Kamesh ;
Winn, Robert A. .
JOVE-JOURNAL OF VISUALIZED EXPERIMENTS, 2014, (92)
[6]  
Branca RMM, 2014, NAT METHODS, V11, P59, DOI [10.1038/NMETH.2732, 10.1038/nmeth.2732]
[7]   Paracrine Induction of HIF by Glutamate in Breast Cancer: EglN1 Senses Cysteine [J].
Briggs, Kimberly J. ;
Koivunen, Peppi ;
Cao, Shugeng ;
Backus, Keriann M. ;
Olenchock, Benjamin A. ;
Patel, Hetalben ;
Zhang, Qing ;
Signoretti, Sabina ;
Gerfen, Gary J. ;
Richardson, Andrea L. ;
Witkiewicz, Agnieszka K. ;
Cravatt, Benjamin F. ;
Clardy, Jon ;
Kaelin, William G., Jr. .
CELL, 2016, 166 (01) :126-139
[8]   Regulation of cancer cell metabolism [J].
Cairns, Rob A. ;
Harris, Isaac S. ;
Mak, Tak W. .
NATURE REVIEWS CANCER, 2011, 11 (02) :85-95
[9]   MEASURING THE REDOX STATE OF CELLULAR PEROXIREDOXINS BY IMMUNOBLOTTING [J].
Cox, Andrew G. ;
Winterbourn, Christine C. ;
Hampton, Mark B. .
METHODS IN ENZYMOLOGY, VOL 474: THIOL REDOX TRANSITIONS IN CELL SIGNALING, PT B: CELLULAR LOCALIZATION AND SIGNALING, 2010, 474 :51-66
[10]   Systemic depletion of L-cyst(e)ine with cyst(e)inase increases reactive oxygen species and suppresses tumor growth [J].
Cramer, Shiro L. ;
Saha, Achinto ;
Liu, Jinyun ;
Tadi, Surendar ;
Tiziani, Stefano ;
Yan, Wupeng ;
Triplett, Kendra ;
Lamb, Candice ;
Alters, Susan E. ;
Rowlinson, Scott ;
Zhang, Yan Jessie ;
Keating, Michael J. ;
Huang, Peng ;
DiGiovanni, John ;
Georgiou, George ;
Stone, Everett .
NATURE MEDICINE, 2017, 23 (01) :120-127