| Literature DB >> 33526988 |
Ko-Chao Lee1, Chia-Kung Yen2, Cheng-Nan Chen3, Shun-Fu Chang4, Ying-Chen Lu2, Wen-Shih Huang5,6.
Abstract
Colorectal cancers (CRCs) is the most commonly diagnosed and deadly cancer types in the world. Despite advances in chemotherapy for CRCs, drug resistance remains a major challenge to high incurable and eventually deadly rates for patients. CPT-11 is one of the current chemotherapy agents for CRC patients and the CPT-11 resistance development of CRCs is also inevitable. Recently, accumulating data has suggested that DNA repair system might be an inducer of chemotherapy resistance in cancer cells. Thus, this study was aimed to examine whether MutS homolog (MSH) 2, one member of DNA repair system, plays a role to affect the cytotoxicity of CPT-11 to CRCs. Human DLD-1 CRC cells were used in this study. It was shown that MSH2 gene and protein expression could be upregulated in DLD-1 cells under CPT-11 treatment and this upregulation subsequently attenuates the sensitivity of DLD-1 cells to CPT-11. Moreover, ERK1/2 and Akt signaling and AP-1 transcription factor have been found to modulate these effects. These results elucidate the drug resistance role of MSH2 upregulation in the CPT-11-treated DLD-1 CRC cells. Our findings may provide a useful thought for new adjuvant drug development by controlling the DNA repair system. © The author(s).Entities:
Keywords: CPT-11; Colorectal cancer; DNA topoisomerases; Drug resistance; MutS homolog 2
Year: 2021 PMID: 33526988 PMCID: PMC7847627 DOI: 10.7150/ijms.52620
Source DB: PubMed Journal: Int J Med Sci ISSN: 1449-1907 Impact factor: 3.738