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Targeting regulation of tryptophan metabolism for colorectal cancer therapy: a systematic review

期刊

RSC ADVANCES
卷 9, 期 6, 页码 3072-3080

出版社

ROYAL SOC CHEMISTRY
DOI: 10.1039/c8ra08520j

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资金

  1. Key Program of Natural Science Foundation of State [81830110, 81430093, 81373930, 81673586, 81703685, 81302905, 81503386]
  2. National Key Subject of Drug Innovation [2015ZX09101043-005, 2015ZX09101043-011]
  3. TCM State Administration Subject of Public Welfare [2015468004]
  4. Major Projects of Application Technology Research and Development Plan in Heilongjiang Province [GX16C003]
  5. Specialized Research Fund for the Doctoral Program of Higher Education [20132327130001, 20122327120006]
  6. University Nursing Program for Young Scholars with Creative Talents in Heilongjiang Province [UNPYSCT-2016213, UNPYSCT-2015118, UNPYSCT-2016212]
  7. Young Talent Lift Engineering Project of China Association of Traditional Chinese Medicine [QNRC2-B06]
  8. Outstanding Talents Foundation of Heilongjiang University of Chinese Medicine [2018jc01]
  9. Doctoral Innovation Fund of Heilongjiang University of Chinese Medicine [2018bs02]
  10. Application Technology and Development of Youth Talents Project in Harbin [2014RFQXJ116]
  11. Chinese Postdoctoral Science Foundation [2017M621319b]
  12. Returned Overseas Scholars Program of Heilongjiang Province [2017QD0025]
  13. Natural Science Foundation of Heilongjiang Province of China [QC2018117]

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Colorectal cancer (CRC) is one of the most malignant cancers resulting from abnormal metabolism alterations. As one of the essential amino acids, tryptophan has a variety of physiological functions, closely related to regulation of immune system, central nervous system, gastrointestinal nervous system and intestinal microflora. Colorectal cancer, a type of high-grade malignancy disease, stems from a variety of factors and often accompanies inflammatory reactions, dysbacteriosis, and metabolic disorders. Colorectal cancer accompanies inflammation and imbalance of intestinal microbiota and affects tryptophan metabolism. It is known that metabolites, rate-limiting enzymes, and ARH in tryptophan metabolism are associated with the development of CRC. Specifically, IDO1 may be a potential therapeutic target in colorectal cancer treatment. Furthermore, the reduction of tryptophan amount is proportional to the poor quality of life for colorectal cancer patients. This paper aims to discuss the role of tryptophan metabolism in a normal organism and investigate the relationship between this amino acid and colorectal cancer. This study is expected to provide theoretical support for research related to targeted therapy for colorectal cancer. Furthermore, strategies that modify tryptophan metabolism, effectively inhibiting tumor progression, may be more effective for CRC treatment.

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