SETD8 promotes glycolysis in colorectal cancer via regulating HIF1α/HK2 axis

Glycolysis is one of the factors influencing cancer cell growth and metastasis. Here, we aimed to investigate the role of SETD8 gene, which is a pro-oncogene. Using bioinformatics tools including Ualcan, Timer, GEPIA, and PrognoScan to study the expression of SETD8 in colorectal cancer, we found that SETD8 expression was higher in colon cancer tissues than that in normal tissues. Higher levels of SETD8 predicted poorer survival of patients. This piqued our interest, so we transfected SETD8 knockdown and overexpression plasmids into colorectal cancer cells and found that SETD8 overexpression enhanced proliferation and glycolysis in colon cancer cells, while SETD8 knockdown decreased cell proliferation and glycolysis. Mechanistically, we examined the expression of HIF1α and HK2 protein by western-blot assay and found that SETD8 activated the HIF1α/HK2 pathway. Then, we treated SETD8-overexpressed cells with HIF1α inhibitor and found that the pro-tumor growth and glycolytic effects of SETD8 were reversed, indicating that SETD8 promoted the growths of colorectal cancer cells by upregulating the HIF1α /HK2 pathway.