Glycolysis promotes the progression of pancreatic cancer and reduces cancer cell sensitivity to gemcitabine.

• Expression of some GRGs was significantly associated with the prognosis or progression of pancreatic cancer. • Pancreatic cancer cell death was enhanced following inhibition of glycolysis. • The sensitivity of cancer cells to GEM was elevated by 2-DG. • A prognostic model involving GRGs should be helpful for pancreatic cancer early diagnosis and treatment. Previous studies have reported that increased glycolytic activity enhances chemotherapy resistance in some types of malignancies. However, whether glycolysis influences the curative effect of gemcitabine (GEM) on pancreatic cancer (PC) cells remains unclear. The aim of this study was to investigate the status of glycolysis in PC and its association with tolerance to GEM. Data from The Cancer Genome Atlas (TCGA) were used to analyze the correlation between glycolysis-related gene (GRG) expression and PC progression and prognosis. 2-Deoxy-D-glucose (2-DG) was applied to assess the effect of glycolysis inhibition on PC cell death and GEM tolerance. Expression of some GRGs, such as HK1, GAPDH, PKM2, and LDHA, was significantly associated with the prognosis of PC. Furthermore, HK1, PKLR, and LDHA expression correlated positively with PC progression. Further analysis revealed that cancer cell death was markedly enhanced following glycolysis inhibition and that the sensitivity of cancer cells to GEM was notably increased in the presence of 2-DG. Our findings indicate that abnormally increased glycolytic activity promotes the development of PC and enhances drug tolerance to GEM. 2-DG combined with GEM is a potential therapy for PC. [ABSTRACT FROM AUTHOR]