Transcriptional dysregulation of TRIM29 promotes colorectal cancer carcinogenesis via pyruvate kinase-mediated glucose metabolism

Jing Han; Zitong Zhao; Nan Zhang; Yang Yang; Liying Ma; Li Feng; Xue Zhang; Jing Zuo; Zhisong Fan; Yudong Wang; Yongmei Song; Guiying Wang

doi:doi:10.18632/aging.202414

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Research Paper Volume 13, Issue 4 pp 5034—5054

Transcriptional dysregulation of TRIM29 promotes colorectal cancer carcinogenesis via pyruvate kinase-mediated glucose metabolism

Figure 6. TRIM29 regulates glycolytic metabolism and the aggressive phenotype in CRC by regulating PKM1. (A, B) After transfection with NC or Si2 in SW480 and HT29 cell lines, (A) The extracellular acidification rate (ECAR) and (B) the oxygen consumption rate (OCR) of cells was measured. (C–F) Cells transfected with GV230 vector plus Ez-M98 vector, TRIM29 plasmid plus Ez-M98 vector, TRIM29 plasmid plus PKM1 plasmid. (C) The ECAR and (D) OCR of cells were measured. (E) Growth was determined using the RTCA-MP system. (F) Migration and invasion were measured using a transwell assay. The statistical analysis was performed using the two-tailed Student’s t-test. **P < 0.01, ***P < 0.001. Every experiment repeated at least 3 times.