Transcriptional Suppression of miR-29b-1/miR-29a Promoter by c-Myc, Hedgehog, and NF-kappaB
Document Type
Article
Publication Date
8-1-2010
Description
MicroRNAs regulate pathways contributing to oncogenesis, and thus the mechanisms causing dysregulation of microRNA expression in cancer are of significant interest. Mature mir-29b levels are decreased in malignant cells, and this alteration promotes the malignant phenotype, including apoptosis resistance. However, the mechanism responsible for mir-29b suppression is unknown. Here, we examined mir-29 expression from chromosome 7q32 using cholangiocarcinoma cells as a model for mir-29b downregulation. Using 5′ rapid amplification of cDNA ends, the transcriptional start site was identified for this microRNA locus. Computational analysis revealed the presence of two putative E-box (Myc-binding) sites, a Gli-binding site, and four NF-κB-binding sites in the region flanking the transcriptional start site. Promoter activity in cholangiocarcinoma cells was repressed by transfection with c-Myc, consistent with reports in other cell types. Treatment with the hedgehog inhibitor cyclopamine, which blocks smoothened signaling, increased the activity of the promoter and expression of mature mir-29b. Mutagenesis analysis and gel shift data are consistent with a direct binding of Gli to the mir-29 promoter. Finally, activation of NF-κB signaling, via ligation of Toll-like receptors, also repressed mir-29b expression and promoter function. Of note, activation of hedgehog, Toll-like receptor, and c-Myc signaling protected cholangiocytes from TRAIL-induced apoptosis. Thus, in addition to c-Myc, mir-29 expression can be suppressed by hedgehog signaling and inflammatory pathways, both commonly activated in the genesis of human malignancies.
Citation Information
Mott, Justin L.; Kurita, Satoshi; Cazanave, Sophie C.; Bronk, Steven F.; Werneburg, Nathan W.; and Fernandez-Zapico, Martin E.. 2010. Transcriptional Suppression of miR-29b-1/miR-29a Promoter by c-Myc, Hedgehog, and NF-kappaB. Journal of Cellular Biochemistry. Vol.110(5). 1155-1164. https://doi.org/10.1002/jcb.22630 PMID: 20564213 ISSN: 0730-2312