Transcriptional silencing of the DLC-1 tumor suppressor gene by epigenetic mechanism in gastric cancer cells

Kim, Tai Young; Jong, Hyun Soon; Song, Sang‐Hyun; Dimtchev, Alexandre; Jeong, Seong‐Jae; Lee, Sang Eun; Kim, Tae-You; Kim, Noe Kyeong; Jung, Mira; Bang, Yung‐Jue

doi:10.1038/sj.onc.1206573

Cited by 101 publications

(92 citation statements)

References 38 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We also showed that DLC1 functions as a TSG in NPC and esophageal carcinoma cells. As DLC1 methylation has not been reported in these three tumors before, our results add more candidates to the reported list of cancers (liver, breast, colon, gastric, lung and prostate) with epigenetic abnormalities of this TSG (Kim et al, 2003;Plaumann et al, 2003;Wong et al, 2003;Yuan et al, 2003aYuan et al, , b, 2004. Interestingly, in one of our independent studies screening for downregulated genes in NPC cell lines using whole-genomic microarray expression profiling combined with pharmacologic demethylation, DLC1 was also identified as one of the downregulated target genes (Tao et al, manuscript in preparation).…”

Section: Discussionsupporting

confidence: 66%

“…DLC1 was reported to be a functional TSG frequently inactivated by promoter methylation in multiple carcinomas (Kim et al, 2003;Plaumann et al, 2003;Wong et al, 2003;Yuan et al, 2003aYuan et al, , b, 2004. DLC1 is located at 8p22 -a region where we also detected heterozygous deletion in some esophageal cell lines by conventional CGH (Tang et al, 2001), but no study of DLC1 has been performed in esophageal carcinoma yet.…”

Section: Resultsmentioning

confidence: 99%

“…It has high sequence similarity (86%) with the rat p122RhoGAP, a GTPase-activating protein for the Rho family of proteins involved in cell cytoskeleton organization and other functions (Homma and Emori, 1995;Etienne-Manneville and Hall, 2002;Moon and Zheng, 2003). More recent studies have demonstrated that DLC1 is an important TSG, being inactivated by aberrant promoter methylation in multiple carcinomas, including liver, colon, gastric, lung, breast and prostate carcinomas (Kim et al, 2003;Plaumann et al, 2003;Wong et al, 2003;Yuan et al, 2003aYuan et al, , b, 2004, while no study has been performed for NPC yet. Here, we report on the epigenetic alterations of DLC1 in NPC and other tumors (esophageal and cervical carcinomas) which have not been studied for this gene.…”

mentioning

confidence: 99%

See 2 more Smart Citations

The major 8p22 tumor suppressor DLC1 is frequently silenced by methylation in both endemic and sporadic nasopharyngeal, esophageal, and cervical carcinomas, and inhibits tumor cell colony formation

Seng¹,

Low²,

et al. 2006

Oncogene

124

118

View full text Add to dashboard Cite

Identification of tumor suppressor genes (TSG) silenced by methylation uncovers mechanisms of tumorigenesis and identifies new epigenetic tumor markers for early cancer detection. Both nasopharyngeal carcinoma (NPC) and esophageal carcinoma are major tumors in Southern China and Southeast Asia. Through expression subtraction of NPC, we identified Deleted in Liver Cancer 1 (DLC1)/ARHGAP7 (NM_006094) -an 8p22 TSG as a major downregulated gene. Although expressed in all normal tissues, DLC1 was silenced or downregulated in 11/12 (91%) NPC, 6/15 (40%) esophageal, 5/8 (63%) cervical and 3/9 (33%) breast carcinoma cell lines. No genetic deletion of DLC1 was detected in NPC although a hemizygous deletion at 8p22-11 was found by 1-Mb array-CGH in some cell lines. We then located the functional DLC1 promoter by 5 0 -RACE and promoter activity assays. This promoter was frequently methylated in all downregulated cell lines and in a large collection of primary tumors including 89% (64/72) NPC (endemic and sporadic types), 51% (48/94) esophageal, 87% (7/8) cervical and 36% (5/14) breast carcinomas, but seldom in paired surgical marginal tissues and not in any normal epithelial tissue. The transcriptional silencing of DLC1 could be reversed by 5-aza-2 0 -deoxycytidine or genetic double knock-out of DNMT1 and DNMT3B. Furthermore, ectopic expression of DLC1 in NPC and esophageal carcinoma cells strongly inhibited their colony formation. We thus found frequent epigenetic silencing of DLC1 in NPC, esophageal and cervical carcinomas, and a high correlation of methylation with its downregulation, suggesting a predominant role of epigenetic inactivation. DLC1 appears to be a major TSG implicated in the pathogenesis of these tumors, and should be further tested as a molecular biomarker in patients with these cancers. Oncogene (2007) 26, 934-944.

show abstract

Section: Discussionsupporting

confidence: 66%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

The major 8p22 tumor suppressor DLC1 is frequently silenced by methylation in both endemic and sporadic nasopharyngeal, esophageal, and cervical carcinomas, and inhibits tumor cell colony formation

Seng¹,

Low²,

et al. 2006

Oncogene

124

118

View full text Add to dashboard Cite

show abstract

“…In addition, DNA methylation and the chromatin condensation of integrin aL were detected in fibroblasts, and were suggested to contribute to the tissue-specific expression of integrin aL (Akama et al, 1997;Lu et al, 2002). Previously, we reported that DNA methylation is one of the predominant mechanisms for inactivating various genes, like, TGF-b type I receptor, TIMP-3, p16, COX-2 and DLC-1, during gastric carcinogenesis (Kang et al, 1999;Kang et al, 2000;Song et al, 2000Song et al, , 2001Kim et al, 2003). These findings led us to investigate whether integrin a4 expression could be regulated by DNA methylation, because integrin a4 expression is very low in our gastric carcinoma cells (Figure 1a).…”

Section: Discussionmentioning

confidence: 99%

Aberrant methylation of integrin α4 gene in human gastric cancer cells

et al. 2004

Self Cite

View full text Add to dashboard Cite

Integrins are adhesion receptors that mediate both cellextracellular matrix and cell-cell interactions. It has also been reported that the loss of integrin a4 expression might be associated with metastasis in several cancers. However, the molecular mechanism for loss of their expression in cancers has not been explored. In the present study, we found that the integrin a4 expression is lost in human gastric cancer cell lines and that this is recovered by treatment with DNA methyltransferase inhibitor, implying transcriptional silencing by DNA methylation. Methylation-specific PCR (MSP) and bisulfite genomic DNA sequencing demonstrated the CpG methylationdependent silencing of integrin a4 expression in eight of nine (88.8%) gastric cancer cell lines and in 84.7% of 46 primary tumors. We also investigated whether the restoration of integrin a4 in integrin a4-inactivated cells affects their ability to invade extracellular matrix, using matrigel assays. Interestingly, integrin a4-stable transfectants had markedly less invasive ability than the parental cells. Taken together, these results suggest that the transcriptional repression of the integrin a4 gene is caused by aberrant DNA methylation, and that this may play an important role in human gastric carcinogenesis.

show abstract

“…5 The promoter hypermethylation of multiple tumor suppressor genes resulting in gene silencing has been recognized as an important mechanism in gastrointestinal carcinogenesis. [6][7][8][9][10][11][12][13][14][15] In a previous study, TSPYL5 was identified as one of the genes induced after treatment with DNA methylation and histone deacetylation inhibitors in glioma cell lines using microarray analysis. 16 The TSPYL5 showed a high frequency of DNA methylation-mediated silencing in both glioma cell lines and primary glial tumors.…”

mentioning

confidence: 99%

Gene silencing of TSPYL5 mediated by aberrant promoter methylation in gastric cancers

Jung

Park

Bang

et al. 2008

Laboratory Investigation

Self Cite

View full text Add to dashboard Cite

DNA methylation is crucial for normal development, but gene expression altered by DNA hypermethylation is often associated with human diseases, especially cancers. The gene TSPYL5, encoding testis-specific Y-like protein, was previously identified in microarray screens for genes induced by the inhibition of DNA methylation and histone deacetylation in glioma cell lines. The TSPYL5 showed a high frequency of DNA methylation-mediated silencing in both glioma cell lines and primary glial tumors. We now report that TSPYL5 is also inactivated by DNA methylation and could be a putative epigenetic target gene in gastric cancers. We found that the expression of TSPYL5 mRNA was frequently downregulated and inversely correlated with DNA methylation in seven out of nine gastric cancer cell lines. TSPYL5 mRNA expression was also restored after treating with a DNA methyltransferase inhibitor. In primary gastric tumors, methylation-specific PCR results in 23 of the 36 (63.9%) cases revealed that the hypermethylation at CpG islands of the TSPYL5 was detectable at a high frequency. Furthermore, TSPYL5 suppressed the growth of gastric cancer cells as demonstrated by a colony formation assay. Thus, strong associations between TSPYL5 expression and hypermethylation were observed, and aberrant methylation at a CpG island of TSPYL5 may play an important role in development of gastric cancers. Epigenetic events are heritable modifications that regulate gene expression and can contribute to cancer development. 1 In particular, changes in DNA methylation are among the most common molecular alterations in human neoplasia, because the hypermethylation of a tumor suppressor gene at a promoter can lead to transcriptional silencing and the loss of gene function. 1-4 Gastric cancer is one of the most common malignancies in the world. 5 The promoter hypermethylation of multiple tumor suppressor genes resulting in gene silencing has been recognized as an important mechanism in gastrointestinal carcinogenesis. [6][7][8][9][10][11][12][13][14][15] In a previous study, TSPYL5 was identified as one of the genes induced after treatment with DNA methylation and histone deacetylation inhibitors in glioma cell lines using microarray analysis. 16 The TSPYL5 showed a high frequency of DNA methylation-mediated silencing in both glioma cell lines and primary glial tumors. A human TSPYL5 encoding testis-specific Y-like protein 5 (TSPYL5) is located on chromosome 8q22.1, but its role in human cancer has not been fully understood. The TSPYL5 protein is a member of TSPYL family that includes TSPYL1, TSPYL2, TSPYL3, TSPYL4, and TSPYL6. TSPYL proteins are also members of the nucleosome assembly protein (NAP) superfamily. The TSPYLs show sequence homology to NAPs, which have a highly conserved domain (the NAP domain) of approximately 180 amino acids. 17,18 The NAP domain is known to be required and sufficient for histone binding. 19 Members of the NAP family of proteins were identified in different systems and were classified with the NAPs based on their sequenc...

show abstract

Transcriptional silencing of the DLC-1 tumor suppressor gene by epigenetic mechanism in gastric cancer cells

Cited by 101 publications

References 38 publications

The major 8p22 tumor suppressor DLC1 is frequently silenced by methylation in both endemic and sporadic nasopharyngeal, esophageal, and cervical carcinomas, and inhibits tumor cell colony formation

The major 8p22 tumor suppressor DLC1 is frequently silenced by methylation in both endemic and sporadic nasopharyngeal, esophageal, and cervical carcinomas, and inhibits tumor cell colony formation

Aberrant methylation of integrin α4 gene in human gastric cancer cells

Gene silencing of TSPYL5 mediated by aberrant promoter methylation in gastric cancers

Contact Info

Product

Resources

About