4.6 Article

Metabolomics study reveals the potential evidence of metabolic reprogramming towards the Warburg effect in precancerous lesions

Journal

JOURNAL OF CANCER
Volume 12, Issue 5, Pages 1563-1574

Publisher

IVYSPRING INT PUBL
DOI: 10.7150/jca.54252

Keywords

metabolic reprogramming; precancerous lesions; metabolomics; the Warburg-like effect; glycolytic enzymes

Categories

Funding

  1. National Natural Science Foundation of China [31670788, 81873711]
  2. Open Fund of Guangdong Key Laboratory of Pharmaceutical Functional Genes [2020B1212060031, 2017B030314021]

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The study found distinct metabolic characteristics in oral precancerous cells and cervical precancerous lesions compared to normal and cancer cells. Enhanced metabolic activity and increased expression of glycolytic enzymes were observed in cervical precancerous lesions, suggesting metabolic reprogramming may contribute to early tumorigenesis.
Background: Most tumors have an enhanced glycolysis flux, even when oxygen is available, called the aerobic glycolysis or the Warburg effect. Metabolic reprogramming promotes cancer progression, and is even related to the tumorigenesis. However, it is not clear whether the observed metabolic changes act as a driver or a bystander in cancer development. Methods: In this study, the metabolic characteristics of oral precancerous cells and cervical precancerous lesions were analyzed by metabolomics, and the expression of glycolytic enzymes in cervical precancerous lesions was evaluated by RT-PCR and Western blot analysis. Results: In total, 115 and 23 metabolites with reliable signals were identified in oral cells and cervical tissues, respectively. Based on the metabolome, oral precancerous cell DOK could be clearly separated from normal human oral epithelial cells (HOEC) and oral cancer cells. Four critical differential metabolites (pyruvate, glutamine, methionine and lysine) were identified between DOK and HOEC. Metabolic profiles could clearly distinguish cervical precancerous lesions from normal cervical epithelium and cervical cancer. Compared with normal cervical epithelium, the glucose consumption and lactate production increased in cervical precancerous lesions. The expression of glycolytic enzymes LDHA, HK II and PKM2 showed an increased tendency in cervical precancerous lesions compared with normal cervical epithelium. Conclusions: Our findings suggest that cell metabolism may be reprogrammed at the early stage of tumorigenesis, implying the contribution of metabolic reprogramming to the development of tumor.

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