Silencing of the VHL tumor-suppressor gene by DNA methylation in renal carcinoma.

Herman, James G.; Latif, Farida; Weng, Yongkai; Lerman, Michael I.; Zbar, Berton; Liu, S; Samid, Dvorit; Duan, Da; Gnarra, James R.; Linehan, W. Marston

doi:10.1073/pnas.91.21.9700

Cited by 1,350 publications

(791 citation statements)

References 24 publications

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“…Thus, the epigenetic inactivation of HOXB13 is independent of the VHL status. This may help us to elucidate the tumorigenic mechanisms of RCCs that lack VHL inactivation, which constitute approximately 40% of the sporadic clear cell RCC cases (Foster et al, 1994;Gnarra et al, 1994;Herman et al, 1994;Shuin et al, 1994Shuin et al, , 1999. Notably, multivariate analysis of the clinicopathological parameters using a logistic regression model showed that HOXB13 methylation correlated significantly with tumor grade and microvessel invasion.…”

Section: Discussionmentioning

confidence: 99%

“…There are more than 30 000 newly diagnosed cases in the USA and 7000 occur in Japan every year. Previous studies revealed that the von Hippel-Lindau (VHL) gene is the major tumor suppressor gene that participates in the development of human RCC, as it is inactivated, mostly by genetic alterations, in about 60% of sporadic RCC cases (Foster et al, 1994;Gnarra et al, 1994;Herman et al, 1994;Shuin et al, 1994Shuin et al, , 1999. However, the tumorigenic mechanisms for the sporadic RCCs that lack VHL gene inactivation and the multi-step processes involved in RCC progression remain unclear.…”

Section: Introductionmentioning

confidence: 99%

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Epigenetic inactivation of the candidate tumor suppressor gene HOXB13 in human renal cell carcinoma

Okuda¹,

Toyota

Ishida

et al. 2005

Oncogene

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Epigenetic alterations like DNA methylation and the resulting inactivation of cancer-related genes often contribute to the development of various cancers. To identify the genes that are silenced by aberrant methylation in renal cell carcinoma (RCC), we subjected two RCC lines to methylated CpG island amplification/representational difference analysis. This identified 27 CpG islands. Combined bisulfite restriction analysis of these CpG islands in primary RCC cases revealed that four were methylated in a tumor-specific manner. One of these was identified as the human homeo-box gene B13 (HOXB13) gene, but the remaining three CpG islands were not associated with known genes. The methylation frequencies of HOXB13 in primary RCC samples and lines were 30 and 73%, respectively. The methylation status of HOXB13 correlated with the loss of its expression both in RCC lines and primary tumors, and methyltransferase inhibitor treatment induced the recovery of its expression. Exogenous expression of HOXB13 in RCC cells that lacked endogenous HOXB13 expression suppressed colony formation and induced apoptotic features. Furthermore, HOXB13 methylation correlated positively with tumor grade and microvessel invasion. These results suggest that HOXB13 is a novel candidate tumor suppressor gene in RCC and that its inactivation may play an important role in both RCC tumorigenesis and progression.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Epigenetic inactivation of the candidate tumor suppressor gene HOXB13 in human renal cell carcinoma

Okuda¹,

Toyota

Ishida

et al. 2005

Oncogene

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“…The response of metastatic RCC to conventional chemotherapy is poor, but characterisation of the molecular pathology of RCC can provide a basis for developing novel therapeutic approaches. This is exemplified by the VHL TSG paradigm in which (a) inactivation of VHL is the most common event in sporadic clear cell RCC (Latif et al, 1993;Foster et al, 1994;Herman et al, 1994;Clifford et al, 1998); (b) VHL inactivation leads to stabilisation of HIF-1 and HIF-2 transcription factors and activation of hypoxic response genes that drive renal tumourigenesis (Maxwell et al, 1999); and (c) inhibitors (for example, tyrosine kinase inhibitors such as sorafenib and sunitinib) of HIF target pathways are active in the treatment of metastatic RCC (Chowdhury et al, 2008). Hence, identification of frequently inactivated RCC TSGs can provide a basis for novel therapeutic interventions.…”

Section: Ct Bstu1mentioning

confidence: 99%

Genome-wide methylation analysis identifies epigenetically inactivated candidate tumour suppressor genes in renal cell carcinoma

et al. 2010

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The detection of promoter region hypermethylation and transcriptional silencing has facilitated the identification of candidate renal cell carcinoma (RCC) tumour suppressor genes (TSGs). We have used a genome-wide strategy (methylated DNA immunoprecipitation (MeDIP) and whole-genome array analysis in combination with highdensity expression array analysis) to identify genes that are frequently methylated and silenced in RCC. MeDIP analysis on 9 RCC tumours and 3 non-malignant normal kidney tissue samples was performed, and an initial shortlist of 56 candidate genes that were methylated by array analysis was further investigated; 9 genes were confirmed to show frequent promoter region methylation in primary RCC tumour samples (KLHL35 (39%), QPCT (19%), SCUBE3 (19%), ZSCAN18 (32%), CCDC8 (35%), FBN2 (34%), ATP5G2 (36%), PCDH8 (58%) and CORO6 (22%)). RNAi knockdown for KLHL35, QPCT, SCUBE3, ZSCAN18, CCDC8 and FBN2 resulted in an anchorage-independent growth advantage. Tumour methylation of SCUBE3 was associated with a significantly increased risk of cancer death or relapse (P ¼ 0.0046). The identification of candidate epigenetically inactivated RCC TSGs provides new insights into renal tumourigenesis.

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“…Anomalies within the p53 tumor suppressor gene are not common in RCC. Mutations in the Von Hippel-Lindau (VHL) tumor-suppressor gene (Latif et al, 1993;Herman et al, 1994;Iliopoulos et al, 1995) or amplification and activation of the tyrosine kinase c-Met (Schmidt et al, 1997;Fischer et al, 1998;Zhuang et al, 1998;Lubensky et al, 1999) have been shown to play critical roles in the development of some RCCs. Despite these advances, the full spectrum of molecular changes that occur in the tumor is far from clear.…”

Section: Introductionmentioning

confidence: 99%

A proteomic analysis reveals the loss of expression of the cell death regulatory gene GRIM-19 in human renal cell carcinomas

et al. 2006

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Silencing of the VHL tumor-suppressor gene by DNA methylation in renal carcinoma.

Cited by 1,350 publications

References 24 publications

Epigenetic inactivation of the candidate tumor suppressor gene HOXB13 in human renal cell carcinoma

Epigenetic inactivation of the candidate tumor suppressor gene HOXB13 in human renal cell carcinoma

Genome-wide methylation analysis identifies epigenetically inactivated candidate tumour suppressor genes in renal cell carcinoma

A proteomic analysis reveals the loss of expression of the cell death regulatory gene GRIM-19 in human renal cell carcinomas

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