4.8 Article

Fusobacterium Nucleatum Promotes the Development of Colorectal Cancer by Activating a Cytochrome P450/Epoxyoctadecenoic Acid Axis via TLR4/Keapl/NRF2 Signaling

CANCER RESEARCH (2021)

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Journal

CANCER RESEARCH
Volume 81, Issue 17, Pages 4485-4498

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/0008-5472.CAN-21-0453

Keywords

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Categories

Oncology

Funding

  1. National Nature Science Foundation of China [81972221, 81730102, 81902422, 81972709, 81920108026, 81871964]
  2. Emerging Cutting-Edge Technology Joint Research projects of Shanghai [SHDC12017112]
  3. Tongji University Subject Pilot Program [1501141201]
  4. Special Construction of Integrated Traditional Chinese Medicine and Western Medicine in Shanghai General Hospital [ZHYY-ZXYJHZX-1-201704]
  5. Social Development Project of Yangzhou science and technology bureau [YZ2020078]
  6. Program of Jiangsu Commission of Health [M2020024]
  7. Shanghai Sailing Program [18YF1419400]
  8. National Ten Thousand Plan Young Top Talents
  9. Shanghai Young Top Talents [QNBJ1701]
  10. Shanghai Science and Technology Development Fund [19410713300]
  11. CSCO-Roche Tumor Research Fund [Y-2019Roche-079]
  12. Fudan University Excellence 2025 Talent Cultivation Plan

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The study uncovers a mechanism by which Fusobacterium nucleatum regulates colorectal cancer metabolism to promote EMT and metastasis through activating the TLR4/Keap1/NRF2 axis to increase CYP2J2 and 12,13-EpOME. These findings provide potential therapeutic targets for patients infected with Fusobacterium nucleatum, highlighting the clinical utility of the CYP2J2/12,13-EpOME axis in colorectal cancer.
Emerging research has revealed regulation of colorectal cancer metabolism by bacteria. Fusobacterium nucleatum (Fn) plays a crucial role in the development of colorectal cancer, however, whether Fit infection modifies metabolism in patients with colorectal cancer remains unknown. Here, LC-MS/MS-based lipidomics identified the upregulation of cytochrome P450 monooxygenases, primarily CYP2J2, and their mediated product 12,13-EpOME in patients with colorectal cancer tumors and mouse models, which increased the invasive and migratory ability of colorectal cancer cells in vivo and in vitro by regulating the epithelial-mesenchymal transition (EMT). Metagenomic sequencing indicated a positive correlation between increased levels of fecal Fn and serum 12,13-EpOME in patients with colorectal cancer. High levels of CYP2J2 in tumor tissues also correlated with high Fn levels and worse overall survival in patients with stage III/IV colorectal cancer. Moreover, Fn was found to activate TLR4/AKT signaling, downregulating Keap1 and increasing NRF2 to promote transcription of CYP2J2. Collectively, these data identify that Fn promotes EMT and metastasis in colorectal cancer by activating a TLR4/Keap1/NRF2 axis to increase CYP2J2 and 12,13-EpOME, which could serve as clinical biomarkers and therapeutic targets for Fn-infected patients with colorectal cancer. Significance This study uncovers a mechanism by which Fusobacterium nucleatum regulates colorectal cancer metabolism to drive metastasis, suggesting the potential biomarker and therapeutic utility of the CYP2J2/12,13-EpOME axis in Fn-infected patients.

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