[PDF][PDF] Specific activation of microRNA-127 with downregulation of the proto-oncogene BCL6 by chromatin-modifying drugs in human cancer cells
Y Saito, G Liang, G Egger, JM Friedman, JC Chuang… - Cancer cell, 2006 - cell.com
Cancer cell, 2006•cell.com
Expression profiling of T24 cells revealed that 17 out of 313 human miRNAs were
upregulated more than 3-fold by simultaneous treatment with the chromatin-modifying drugs
5-aza-2′-deoxycytidine and 4-phenylbutyric acid. One of these, miR-127, is embedded in a
CpG island and is highly induced from its own promoter after treatment. miR-127 is usually
expressed as part of a miRNA cluster in normal cells but not in cancer cells, suggesting that
it is subject to epigenetic silencing. In addition, the proto-oncogene BCL6, a potential target …
upregulated more than 3-fold by simultaneous treatment with the chromatin-modifying drugs
5-aza-2′-deoxycytidine and 4-phenylbutyric acid. One of these, miR-127, is embedded in a
CpG island and is highly induced from its own promoter after treatment. miR-127 is usually
expressed as part of a miRNA cluster in normal cells but not in cancer cells, suggesting that
it is subject to epigenetic silencing. In addition, the proto-oncogene BCL6, a potential target …
Summary
Expression profiling of T24 cells revealed that 17 out of 313 human miRNAs were upregulated more than 3-fold by simultaneous treatment with the chromatin-modifying drugs 5-aza-2′-deoxycytidine and 4-phenylbutyric acid. One of these, miR-127, is embedded in a CpG island and is highly induced from its own promoter after treatment. miR-127 is usually expressed as part of a miRNA cluster in normal cells but not in cancer cells, suggesting that it is subject to epigenetic silencing. In addition, the proto-oncogene BCL6, a potential target of miR-127, was translationally downregulated after treatment. These results suggest that DNA demethylation and histone deacetylase inhibition can activate expression of miRNAs that may act as tumor suppressors.
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