Curcumin induces reâexpression of BRCA1 and suppression of γ synuclein by modulating DNA promoter methylation in breast cancer cell lines.
[No authors listed]
摘要
Restoration of normal DNA promoter methylation and expression states of cancerârelated genes may be an option for the prevention as well as the treatment of several types of cancer. Constitutional promoter methylation of BRCA1 DNA repair associated (BRCA1) gene is linked with a high risk of developing breast and ovarian cancer. Furthermore, hypomethylation of the protoâoncogene γ synuclein (SNCG) is associated with the metastasis of breast and ovarian cancer and reduced diseaseâfree survival (DFS). In the present study, we evaluated the potential of curcumin to reâexpress hypermethylated BRCA1 and to suppress hypomethylated SNCG in tripleânegative breast cancer (TNBC) cell line HCCâ38, the estrogen receptorânegative/progesterone receptorânegative (ERâ/PRâ) cell line UACCâ3199, and the ER+/PR+ cell line T47D. The cells were treated with 5 and 10 µM curcumin for 6 days and with 5âazaâ2'âdeoxycytidine (5'âazaâCdR) for 48 h. Methylationâspecific PCR and bisulfite pyrosequencing assays were used to assess DNA promoter methylation while gene expression levels were analyzed using quantitative realâtime PCR and immunoblotting. We found that curcumin treatment restored BRCA1 gene expression by reducing the DNA promoter methylation level in HCCâ38 and UACCâ3199 cells and that it suppressed the expression of SNCG by inducing DNA promoter methylation in T47D cells. Notably, 5'âazaâCdR restored BRCA1 gene expression only in UACCâ3199, and not in HCCâ38 cells. Curcuminâinduced hypomethylation of the BRCA1 promoter appears to be realized through the upregulation of the tenâeleven translocation 1 (TET1) gene, whereas curcuminâinduced hypermethylation of SNCG may be realized through the upregulation of the DNA methyltransferase 3 (DNMT3) and the downregulation of TET1. Notably, miRâ29b was found to be reversely expressed compared to TET1 in curcuminâ and 5'âazaâCdRâtreated cells, suggesting its involvement in the regulation of TET1. Overall, our results indicate that curcumin has an intrinsic dual function on DNA promoter methylation. We believe that curcumin may be considered a promising therapeutic option for treating TNBC patients in addition to preventing breast and ovarian cancer, particularly in cancerâfree females harboring methylated BRCA1.
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基因功能
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原始数据
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文献解读
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