Frequent epigenetic inactivation of DICKKOPF family genes in human gastrointestinal tumors

Abstract

Activation of Wnt signaling has been implicated in tumorigenesis, and epigenetic silencing of Wnt antagonist genes has been detected in various cancers. In the present study, we examined the expression and methylation of DICKKOPF ( DKK ) family genes in gastrointestinal cancer cell lines. We found that all known DKK genes were frequently silenced in colorectal cancer (CRC) cells ( DKK1 , 3/9, 33%; DKK2 , 8/9, 89%; DKK3 , 5/9, 56% and DKK4 , 5/9, 56%), but not in normal colon mucosa. DKK1 , - 2 and - 3 have 5′ CpG islands, and show an inverse relation between expression and methylation. DKK methylation also was frequently observed in gastric cancer (GC) cell lines ( DKK1 , 6/16, 38%; DKK2 , 15/16, 94% and DKK3 , 10/16, 63%), but was seen less frequently in hepatocellular carcinoma and pancreatic cancer cell lines. DKK s also were frequently methylated in primary CRCs ( DKK1 , 7/58, 12%; DKK2 , 45/58, 78% and DKK3 , 12/58, 21%) and GCs ( DKK1 , 15/31, 48%; DKK2 , 26/31, 84% and DKK3 , 12/31, 39%). Against a background of CTNNB1 or APC mutations, Dickkopfs (Dkks) were less effective inhibitors of Wnt signaling than secreted frizzled-related proteins, though over-expression of Dkks suppressed colony formation of CRC cells with such mutations. Our results demonstrate that DKK s are frequent targets of epigenetic silencing in gastrointestinal tumors, and that loss of DKK s may facilitate tumorigenesis through β-catenin/T-cell factor-independent mechanisms.