1.Triptolide downregulates human GD3 synthase (hST8Sia I) gene expression in SK-MEL-2 human melanoma cells.
Haw Young KWON ; Seok Jo KIM ; Cheorl Ho KIM ; Sung Wook SON ; Kyoung Sook KIM ; Jai Heon LEE ; Su Il DO ; Young Choon LEE
Experimental & Molecular Medicine 2010;42(12):849-855
In this study, we have shown that gene expression of human GD3 synthase (hST8Sia I) is suppressed by triptolide (TPL) in human melanoma SK-MEL-2 cells. To elucidate the mechanism underlying the downregulation of hST8Sia I gene expression in TPL-treated SK-MEL-2 cells, we characterized the TPL-inducible promoter region within the hST8Sia I gene using luciferase constructs carrying 5'-deletions of the hST8Sia I promoter. Functional analysis of the 5'-flanking region of the hST8Sia I gene demonstrated that the -1146 to -646 region, which contains putative binding sites for transcription factors c-Ets-1, CREB, AP-1 and NF-kappaB, functions as the TPL-inducible promoter of hST8Sia I in SK-MEL-2 cells. Site-directed mutagenesis and ChIP analysis indicated that the NF-kappaB binding site at -731 to -722 is crucial for TPL-induced suppression of hST8Sia I in SK-MEL-2 cells. This suggests that TPL induces down-regulation of hST8Sia I gene expression through NF-kappaB activation in human melanoma cells.
Cell Proliferation/drug effects
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Diterpenes/*pharmacology
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Down-Regulation
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Epoxy Compounds/pharmacology
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Genes, Reporter
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Humans
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NF-kappa B/metabolism
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Phenanthrenes/*pharmacology
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Promoter Regions, Genetic
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Sialyltransferases/*biosynthesis/genetics
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Tumor Cells, Cultured