4.7 Article

Synthetic Essentiality of Tryptophan 2,3-Dioxygenase 2 in APC-Mutated Colorectal Cancer

CANCER DISCOVERY (2022)

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Journal

CANCER DISCOVERY
Volume 12, Issue 7, Pages 1702-1717

Publisher

AMER ASSOC CANCER RESEARCH
DOI: 10.1158/2159-8290.CD-21-0680

Keywords

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Categories

Oncology

Funding

  1. MD Anderson SPORE in Gastrointestinal Cancer
  2. NIH/NCI [1R01 CA231349, R01 CA231360]
  3. NIH T32 Training Grant in Cancer Biology [T32 CA186892]
  4. Cancer Prevention & Research Institute of Texas (CPRIT) Research Training Program [RP170067]
  5. UT Health Science Center at Houston Center for Clinical and Translational Sciences TL1 Program [TL1 TR003169]
  6. CPRIT Recruitment of First-Time Tenure-Track Faculty Award [RR190021]
  7. NCI Cancer Center Support Grant [P30 CA16672]
  8. United States Public Health Service Cancer Center Support Grant [P30 CA022453]

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This study identifies critical effectors in the maintenance of APC-deficient colorectal cancer and demonstrates the relationship between APC/WNT pathway and kynurenine pathway signaling. It further determines the tumor-associated macrophage biology in APC-deficient colorectal cancer, informing genotype-specific therapeutic targets and the use of TDO2 inhibitors.
Inactivation of adenomatous polyposis coli (APC) is common across many cancer types and serves as a critical initiating event in most sporadic colorectal cancers. APC deficiency activates WNT signaling, which remains an elusive target for cancer therapy, prompting us to apply the synthetic essentiality framework to identify druggable vulnerabilities for APC-deficient cancers. Tryptophan 2,3-dioxygenase 2 (TDO2) was identified as a synthetic essential effector of APCdeficient colorectal cancer. Mechanistically, APC deficiency results in the TCF4/beta-catenin-mediated upregulation of TDO2 gene transcription. TDO2 in turn activates the Kyn-AhR pathway, which increases glycolysis to drive anabolic cancer cell growth and CXCL5 secretion to recruit macrophages into the tumor microenvironment. Therapeutically, APC-deficient colorectal cancer models were susceptible to TDO2 depletion or pharmacologic inhibition, which impaired cancer cell proliferation and enhanced antitumor immune profiles. Thus, APC deficiency activates a TCF4-TDO2-AhR-CXCL5 circuit that affects multiple cancer hallmarks via autonomous and nonautonomous mechanisms and illuminates a genotype-specific vulnerability in colorectal cancer. SIGNIFICANCE: This study identifies critical effectors in the maintenance of APC-deficient colorectal cancer and demonstrates the relationship between APC/WNT pathway and kynurenine pathway signaling. It further determines the tumor-associated macrophage biology in APC-deficient colorectal cancer, informing genotype-specific therapeutic targets and the use of TDO2 inhibitors.

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