Differential epigenetic profiles induced by sodium selenite in breast cancer cells

Selenium (Se) was a potential anticancer micronutrient with proposed epigenetic effect. However, the Se-induced epigenome in breast cancer cells was yet to be studied. The profiles of DNA methylation, microRNA (miRNA), long non-coding RNA (lncRNA), and message RNA (mRNA) in breast cancer cells treat...

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Veröffentlicht in:Journal of trace elements in medicine and biology 2021-03, Vol.64, p.126677-126677, Article 126677
Hauptverfasser: Liang, Zhuo-Zhi, Zhu, Rui-Mei, Li, Yue-Lin, Jiang, Hong-Mei, Li, Ruo-Bi, Wang, Qing, Tang, Lu-Ying, Ren, Ze-Fang
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Sprache:eng
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Zusammenfassung:Selenium (Se) was a potential anticancer micronutrient with proposed epigenetic effect. However, the Se-induced epigenome in breast cancer cells was yet to be studied. The profiles of DNA methylation, microRNA (miRNA), long non-coding RNA (lncRNA), and message RNA (mRNA) in breast cancer cells treated with sodium selenite were examined by microarrays. We verified the epigenetic modifications by integrating their predicted target genes and differentially expressed mRNAs. The epigenetically regulated genes were further validated in a breast cancer cohort by associating with tumor progression. We conducted a series of bioinformatics analyses to assess the biological function of these validated genes and identified the critical genes. The Se-induced epigenome regulated the expression of 959 genes, and 349 of them were further validated in the breast cancer cohort. Biological function analyses suggested that these validated genes were enriched in several cancer-related pathways, such as PI3K/Akt and metabolic pathways. Based on the degrees of expression change, hazard ratio difference, and connectivity, NEDD4L and FMO5 were identified as the critical genes. These results confirmed the epigenetic effects of sodium selenite and revealed the epigenetic profiles in breast cancer cells, which would help understand the mechanisms of Se against breast cancer.
ISSN:0946-672X
1878-3252
DOI:10.1016/j.jtemb.2020.126677