期刊
ONCOTARGET
卷 6, 期 12, 页码 10195-10206出版社
IMPACT JOURNALS LLC
DOI: 10.18632/oncotarget.3555
关键词
ING5; miR-193a-3p; chemoresistance; bladder cancer; protein acetylation
资金
- National Natural Science Foundation of China [81472638, 81171996, 81272289, 81200975]
- Young Outstanding Scholarship Foundation of Anhui Medical University
- Wujieping Medical Foundation [320.6750.13252]
As the major barrier to curative cancer chemotherapy, chemoresistance presents a formidable challenge to both cancer researchers and clinicians. We have previously shown that the bladder cancer (BCa) cell line 5637 is significantly more sensitive to the cytoxicity of five chemotherapeutic agents than H-bc cells. Using an RNA-seq-based omic analysis and validation at both the mRNA and protein levels, we found that the inhibitor of growth 5 (ING5) gene was upregulated in 5637 cells compared with H-bc cells, indicating that it has an inhibitory role in BCa chemoresistance. siRNA-mediated inhibition of ING5 increased the chemoresistance and inhibited the DNA damage response pathway in 5637 cells. Conversely, forced expression of EGFP-ING5 decreased the chemoresistance of and activated the DNA damage response pathway in H-bc cells. We also showed that ING5 gene expression is inhibited by miR-193a-3p and is instrumental in miR-193a-3p's role in activating BCa chemoresistance. Our results demonstrate both the role and mechanism of inhibition of BCa chemoresistance by ING5.
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