Gene Expression Profiles Associated with Radio-Responsiveness in Locally Advanced Rectal Cancer.
Jeeyong LeeJunhye KwonDaYeon KimMisun ParkKwang Seok KimInHwa BaeHyunkyung KimJoon-Seog KongYounjoo KimUiSup ShinEun Ju KimPublished in: Biology (2021)
LARC patients were sorted according to their radio-responsiveness and patient-derived organoids were established from the respective cancer tissues. Expression profiles for each group were obtained using RNA-seq. Biological and bioinformatic analysis approaches were used in deciphering genes and pathways that participate in the radio-resistance of LARC. Thirty candidate genes encoding proteins involved in radio-responsiveness-related pathways, including the immune system, DNA repair and cell-cycle control, were identified. Interestingly, one of the candidate genes, cathepsin E (CTSE), exhibited differential methylation at the promoter region that was inversely correlated with the radio-resistance of patient-derived organoids, suggesting that methylation status could contribute to radio-responsiveness. On the basis of these results, we plan to pursue development of a gene chip for diagnosing the radio-responsiveness of LARC patients, with the hope that our efforts will ultimately improve the prognosis of LARC patients.
Keyphrases
- gene expression
- cell cycle
- end stage renal disease
- dna repair
- rna seq
- rectal cancer
- dna methylation
- locally advanced
- newly diagnosed
- genome wide
- ejection fraction
- peritoneal dialysis
- chronic kidney disease
- cell proliferation
- prognostic factors
- high throughput
- clinical trial
- neoadjuvant chemotherapy
- transcription factor
- copy number
- quality improvement
- lymph node
- genome wide analysis