PRDX6 Drives Breast Cancer Progression Through Mitochondrial Biosynthesis and Oxidative Phosphorylation

被引:0
作者
Dai, Mei [1 ]
Zhang, Danhua [1 ,2 ]
机构
[1] Cent South Univ, Xiangya Hosp 2, Dept Gen Surg, Changsha, Hunan, Peoples R China
[2] Clin Res Ctr Breast Dis Hunan Prov, Changsha, Hunan, Peoples R China
关键词
breast cancer; mitochondria; oxidative phosphorylation (OXPHOS); PRDX6; tumorigenesis; CELL-CYCLE ARREST; PROMOTES; OVEREXPRESSION; RESISTANCE; PARADIGMS; PATHWAY; DAMAGE;
D O I
10.1002/cam4.71005
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
BackgroundPeroxiredoxin 6 (PRDX6) scavenges reactive oxygen species (ROS) and plays a key role in antioxidant defense. Although PRDX6 is involved in various cancers, its role in breast cancer (BRCA) remains unclear.MethodsCell proliferation was assessed using CCK-8, EdU staining, and colony formation assays. Migration and invasion were evaluated via wound-healing and transwell assays. ROS levels and mitochondrial membrane potential were measured by fluorescence microscopy or flow cytometry. Oxidative phosphorylation (OXPHOS) activity was determined by ATP production and NAD+/NADH ratio. Mitochondria were visualized by TEM, and mitochondrial complex subunits were detected by quantitative real-time PCR and Western blotting. In vivo effects were evaluated using a xenograft tumor model.ResultsAlthough PRDX6 was downregulated in BRCA overall, it showed elevated expression in aggressive subtypes and advanced-stage tumors, correlating with poor prognosis. Overexpression of PRDX6 enhanced BRCA cell proliferation, migration, and invasion. PRDX6 reduced ROS levels, upregulated mitochondrial transcription factor A (TFAM) expression, and promoted mitochondrial complex subunit expression and OXPHOS. Inhibition of TFAM led to a decrease in the expression of some of the mitochondrial complex subunits, which reversed the pro-carcinogenic phenotype of the tumor. PRDX6 also promoted tumor growth in vivo.ConclusionPRDX6 maintains intracellular homeostasis by reducing ROS and promotes mitochondrial biogenesis and OXPHOS through TFAM-dependent and -independent pathways, driving BRCA progression.
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页数:12
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共 44 条
[1]   Oxidative Phosphorylation as an Emerging Target in Cancer Therapy [J].
Ashton, Thomas M. ;
McKenna, W. Gillies ;
Kunz-Schughart, Leoni A. ;
Higgins, Geoff S. .
CLINICAL CANCER RESEARCH, 2018, 24 (11) :2482-2490
[2]  
Braden AM, 2014, CURR PHARM DESIGN, V20, P4879
[3]   Identification of the functional role of peroxiredoxin 6 in the progression of breast cancer [J].
Chang, Xin-Zhong ;
Li, Da-Qiang ;
Hou, Yi-Feng ;
Wu, Jiong ;
Lu, Jin-Song ;
Di, Gen-Hong ;
Jin, Wei ;
Ou, Zhou-Luo ;
Shen, Zhen-Zhou ;
Shao, Zhi-Ming .
BREAST CANCER RESEARCH, 2007, 9 (06)
[4]   New paradigms in the repair of oxidative damage in human genome: mechanisms ensuring repair of mutagenic base lesions during replication and involvement of accessory proteins [J].
Dutta, Arijit ;
Yang, Chunying ;
Sengupta, Shiladitya ;
Mitra, Sankar ;
Hegde, Muralidhar L. .
CELLULAR AND MOLECULAR LIFE SCIENCES, 2015, 72 (09) :1679-1698
[5]   Oxidative phosphorylation is a metabolic vulnerability of endocrine therapy and palbociclib resistant metastatic breast cancers [J].
El-Botty, Rania ;
Morriset, Ludivine ;
Montaudon, Elodie ;
Tariq, Zakia ;
Schnitzler, Anne ;
Bacci, Marina ;
Lorito, Nicla ;
Sourd, Laura ;
Huguet, Lea ;
Dahmani, Ahmed ;
Painsec, Pierre ;
Derrien, Heloise ;
Vacher, Sophie ;
Masliah-Planchon, Julien ;
Raynal, Virginie ;
Baulande, Sylvain ;
Larcher, Thibaut ;
Vincent-Salomon, Anne ;
Dutertre, Guillaume ;
Cottu, Paul ;
Gentric, Geraldine ;
Mechta-Grigoriou, Fatima ;
Hutton, Scott ;
Driouch, Keltouma ;
Bieche, Ivan ;
Morandi, Andrea ;
Marangoni, Elisabetta .
NATURE COMMUNICATIONS, 2023, 14 (01)
[6]   Oxidative Phosphorylation Is a Metabolic Vulnerability in Chemotherapy-Resistant Triple-Negative Breast Cancer [J].
Evans, Kurt W. ;
Yuca, Erkan ;
Scott, Stephen S. ;
Zhao, Ming ;
Arango, Natalia Paez ;
Pico, Christian X. Cruz ;
Saridogan, Turcin ;
Shariati, Maryam ;
Class, Caleb A. ;
Bristow, Christopher A. ;
Vellano, Christopher P. ;
Zheng, Xiaofeng ;
Gonzalez-Angulo, Ana Maria ;
Su, Xiaoping ;
Tapia, Coya ;
Chen, Ken ;
Akcakanat, Argun ;
Lim, Bora ;
Tripathy, Debu ;
Yap, Timothy A. ;
Di Francesco, Maria Emilia ;
Draetta, Giulio F. ;
Jones, Philip ;
Heffernan, Timothy P. ;
Marszalek, Joseph R. ;
Meric-Bernstam, Funda .
CANCER RESEARCH, 2021, 81 (21) :5572-5581
[7]   MiR-199a-3p enhances breast cancer cell sensitivity to cisplatin by downregulating TFAM (TFAM) [J].
Fan, Xuelong ;
Zhou, Shangcheng ;
Zheng, Miao ;
Deng, Xiyun ;
Yi, Yinsha ;
Huang, Tieniu .
BIOMEDICINE & PHARMACOTHERAPY, 2017, 88 :507-514
[8]   Revisited Metabolic Control and Reprogramming Cancers by Means of the Warburg Effect in Tumor Cells [J].
Fukushi, Abekura ;
Kim, Hee-Do ;
Chang, Yu-Chan ;
Kim, Cheorl-Ho .
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES, 2022, 23 (17)
[9]   Mitochondrial transcription factor A contributes to cisplatin resistance in patients with estrogen receptor-positive breast cancer [J].
Gao, Wei ;
Wu, Mei-Hong ;
Wang, Ning ;
Ying, Ming-Zheng ;
Zhang, Ying-Yi ;
Hua, Jing ;
Chuan, Liu ;
Wang, Ya-Jie .
MOLECULAR MEDICINE REPORTS, 2016, 14 (06) :5304-5310
[10]   Targeting OXPHOS and the electron transport chain in cancer; Molecular and therapeutic implications [J].
Greene, John ;
Segaran, Ashvina ;
Lord, Simon .
SEMINARS IN CANCER BIOLOGY, 2022, 86 :851-859