Inactivation of <i>RASSF2A</i> by promoter methylation correlates with lymph node metastasis in nasopharyngeal carcinoma

Zhang, Zhe; Sun, Di; Van, Do Nguyen; Tang, Anzhou; Hu, Li–Fu; Huang, Guangwu

doi:10.1002/ijc.22185

Cited by 82 publications

(90 citation statements)

References 24 publications

(25 reference statements)

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“…The feasibility of using RASSF2A methylation as a biomarker for CRCs, perhaps in combination with other genes, is an area of current research in our laboratory. RASSF2A methylation has also been found in gastric cancer at frequencies ranging from 29 to 79% and in 51% of NPC primary tumours (Endoh et al, 2005;Zhang et al, 2007). In NPC tumours RASSF2A methylation correlates with increased metastatic potential (Zhang et al, 2007).…”

Section: Rassf1mentioning

confidence: 99%

“…RASSF2A methylation has also been found in gastric cancer at frequencies ranging from 29 to 79% and in 51% of NPC primary tumours (Endoh et al, 2005;Zhang et al, 2007). In NPC tumours RASSF2A methylation correlates with increased metastatic potential (Zhang et al, 2007). While RASSF4/AD037 is expressed in a variety of normal tissues, it is lost or downregulated in a variety of tumour-cell lines and primary tumours.…”

Section: Rassf1mentioning

confidence: 99%

“…It is also important to note that in some cell backgrounds (prostate and renal cancer cell lines LNCaP and KRC/Y, respectively) RASSF1C re-expression potently suppressed tumour growth in vitro and in vivo in SCID mice suggesting it too could act as a TSG (Li et al, 2004b). Re-expression of RASSF2A, AD037A and NORE1A also results in suppression of tumour growth in a variety of different tumour types Chen et al, 2003;Vos et al, 2003a, b;Aoyama et al, 2004;Eckfeld et al, 2004;Akino et al, 2005;Zhang et al, 2007). For several RASSF members growth suppression is enhanced by co-transfection of constitutively active Ras proteins (Vos et al, 2000(Vos et al, , 2003a or by artificially forcing membrane localization thereby facilitating interaction with Ras (Eckfeld et al, 2004).…”

Section: Rassf1mentioning

confidence: 99%

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Evaluation of the 3p21.3 tumour-suppressor gene cluster

2007

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Section: Rassf1mentioning

confidence: 99%

Section: Rassf1mentioning

confidence: 99%

Section: Rassf1mentioning

confidence: 99%

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Evaluation of the 3p21.3 tumour-suppressor gene cluster

2007

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“…4) ( Table 3). Inactivation of the RASSF1A and p16 tumor suppressor genes on 3p21 and 9p21 by homozygous deletions and promoter methylation are the most common alterations described in NPC [30][31][32]. 3p and 9p abnormalities have been identified in low-grade dysplastic lesions and normal nasopharyngeal mucosa of individuals at high risk indicating that these genetic changes are early events in the pathogenesis of NPC [10,17,20,33].…”

Section: Molecular Genetic Alterationsmentioning

confidence: 99%

An Update on Epstein-Barr Virus and Nasopharyngeal Carcinogenesis

Perez-Ordoñez

2007

Head and Neck Pathol

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“…[10][11][12] Thus, we thought that epigenetic silencing of tumor suppressor genes might be involved in the tumorigenesis of hepatoblastoma and examined the methylation status of 13 candidate tumor suppressor genes, whose aberrant methylation has previously been shown in various cancers. [13][14][15][16][17][18][19][20][21][22] Conventional methylation-specific PCR (MSP) analysis showed hypermethylation in only 3 of the 13 genes, RASSF1A, SOCS1 (suppressor of cytokine signaling 1) and CASP8 (caspase-8) genes, but not in the remaining 10 genes. We examined the correlation of the methylation status of the 3 genes with various clinical characteristics in a substantial number of hepatoblastoma tumors.…”

mentioning

confidence: 99%

The methylation status of RASSF1A promoter predicts responsiveness to chemotherapy and eventual cure in hepatoblastoma patients

Honda

Haruta

Sugawara

et al. 2008

Intl Journal of Cancer

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Despite the progress of therapy, outcomes of advanced hepatoblastoma patients who are refractory to standard preoperative chemotherapy remain unsatisfactory. To improve the mortality rate, novel prognostic markers are needed for better therapy planning. We examined the methylation status of 13 candidate tumor suppressor genes in 20 hepatoblastoma tumors by conventional methylation-specific PCR (MSP) and found hypermethylation in 3 of the 13 genes. We analyzed the methylation status of these 3 genes (RASSF1A, SOCS1 and CASP8) in 97 tumors and found hypermethylation in 30.9, 33.0 and 15.5%, respectively. Univariate analysis showed that only the methylation status of RASSF1A but not the other 2 genes predicted the outcome, and multivariate analysis showed a weak contribution of RASSF1A methylation to overall survival. Using quantitative MSP, we found RASSF1A methylation in 44.3% of the 97 tumors. CTNNB1 mutation was detected in 67.0% of the 97 tumors. While univariate analysis demonstrated RASSF1A methylation, CTNNB1 mutation and other clinicopathological variables as prognostic factors, multivariate analysis identified RASSF1A methylation (p 5 0.043; relative risk 9.39) and the disease stage (p 5 0.002; relative risk 7.67) but not CTNNB1 mutation as independent prognostic factors. In survival analysis of 33 patients in stage 3B or 4, patients with unmethylated tumor had better overall survival than those with methylated tumor (p 5 0.035). RASSF1A methylation may be a promising moleculargenetic marker to predict the treatment outcome and may be used to stratify patients when clinical trials are carried out. ' 2008 Wiley-Liss, Inc.Key words: RASSF1A; CTNNB1; quantitative MSP; hepatoblastoma; prognostic factor Hepatoblastoma is a rare malignant neoplasm of the liver, with an incidence of 0.5-1.5 per million children. 1 Remarkable progress in clinical outcome has been achieved in the past 20 years due to advances in chemotherapy and surgical procedures; however, the mortality rate remains 20-30% and treatment results in patients in advanced stages who are refractory to standard preoperative chemotherapy regimens are unsatisfactory. 2,3 To improve the mortality of these patients, innovative treatment and potent prognostic markers for better therapy planning are needed. The present clinical factors predicting outcome include the level of alpha-feto protein, histology, disease stage and growth pattern of the tumor. 2-4 Chromosomal gains of 2q, 8q and 20 and high expression of telomerase or PLK1 were shown to be moleculargenetic markers predicting poor outcome 5-8 ; however, none have been proven to be independent prognostic factors by multivariate analysis.We previously reported that RASSF1A (RAS association domain family protein 1) methylation, found in 39% of 39 hepatoblastoma tumors, was correlated with poor outcome by univariate analysis. 9 Nevertheless, the article had some limitations that the number of tumors was not enough, the method used to detect the hypermethylation was suboptimal, and the prognostic signifi...

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Inactivation of RASSF2A by promoter methylation correlates with lymph node metastasis in nasopharyngeal carcinoma

Cited by 82 publications

References 24 publications

Evaluation of the 3p21.3 tumour-suppressor gene cluster

Evaluation of the 3p21.3 tumour-suppressor gene cluster

An Update on Epstein-Barr Virus and Nasopharyngeal Carcinogenesis

The methylation status of RASSF1A promoter predicts responsiveness to chemotherapy and eventual cure in hepatoblastoma patients

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