Frequent hypermethylation of the RASSF1A gene in prostate cancer

Liu, Limin; Yoon, Jung‐Hoon; Dammann, Reinhard; Pfeifer, Gerd P.

doi:10.1038/sj.onc.1205814

Cited by 145 publications

(100 citation statements)

References 38 publications

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“…This possibility led us to investigate the methylation of two additional genes in the 50 prostate cancer samples (Table 2). Data for RASSF1A methylation were obtained from previous work (Liu et al, 2002). The methylation of RAR-beta and RASSF1A was not statistically correlated, although there was a trend for an association (r ¼ 0.26, P ¼ 0.069).…”

Section: Methylation Analysis Of the Er-beta And Rassf1a Promoter Regmentioning

confidence: 99%

“…PCR products were separated on a 2% TBE agarose gel and stained with ethidium bromide, or transferred to a nylon membrane, then hybridized with a labeled probe and visualized by autoradiography. The expression of GAPDH was analysed as a control (Liu et al, 2002).…”

Section: Expression Of Tig1mentioning

confidence: 99%

“…For the analysis of the methylation of the ER-beta gene, methylation-specific primers UER-beta-M (5 0 -GCGTTGGGCGTTTTTGAGATCGTC-3 0 ) and LERbeta-M (5 0 -CAATTATTTCTCGCAACCTCCGCG-3 0 ) or unmethylation-specific primers UER-beta-U (5 0 -GTGTTGGG TGTTTTTGAGATTGTT-3 0 ) and LER-beta-U (5 0 -ACAAT TATTTCTCACAACCTCCACA-3 0 ) were used. The analysis of methylation in the RASSF1A CpG island was carried out by MSP as described previously (Liu et al, 2002). For bisulfite sequencing, 100 ng of bisulfite-treated genomic DNA was amplified with TIG1 sequencing primers: TIG1seqU (5 0 -AGG AGTGGTTTTATGGGGAT-3 0 ) and TIG1seqL1 (5 0 -AACC CGAACCAAAAAA-CAAACA-3 0 ), or with the putative RARE sequencing primers: RareU (5 0 -GTTATTTGTT TAAAAA-GAGTTG-3 0 ) and RareL (5 0 -CAAACAATTC TA-CCTCAACCTC-3 0 ) in the reaction buffer (100 ml) containing dNTPs and Hotstar Taq polymerase at 951C for 15 min and then 40 cycles of 941C for 30 s, 581C (531C for RARE sequencing) for 50 s and 721C for 50 s, followed by a final extension step at 721C for 10 min.…”

Section: Methylation Analysismentioning

confidence: 99%

“…Epigenetic inactivation of tumor suppressor genes through DNA methylation in CpGrich promoter regions contributes to tumorigenesis (Baylin and Herman, 2000;Jones and Baylin, 2002). In prostate cancer, aberrant methylation is involved in the inactivation of various important genes such as E-cadherin, CD44, RASSF1A, GSTP1, the endothelin B receptor, p16, the androgen receptor gene, the retinoic acid receptor beta (RARbeta), the estrogen receptor beta (ER-beta) and the caveolin-1 gene (Lee et al, 1994;Nelson et al, 1997;Cui et al, 2001;Kito et al, 2001;Li et al, 2000Li et al, , 2001Nakayama et al, 2001;Pao et al, 2001;Kuzmin et al, 2002;Liu et al, 2002). When tested, loss of the expression of these genes was associated with CpG island hypermethylation, and expression could be restored after treatment with 5-aza-2 0 -deoxycytidine (5-Aza-CdR), a DNA methyltransferase inhibitor.…”

Section: Introductionmentioning

confidence: 99%

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Methylation of the retinoid response gene TIG1 in prostate cancer correlates with methylation of the retinoic acid receptor beta gene

2003

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Methylation of CpG islands and associated gene silencing may lead to malignant progression, but the mechanisms of CpG island methylation in cancer are unknown. The tazarotene-induced gene 1 (TIG1), also known as retinoid acid (RA) receptor-responsive 1 gene was first identified as an RA-responsive gene and was shown to be downregulated in prostate cancer. Here, we show that this downregulation is caused by the methylation of the promoter and CpG island of TIG1. TIG1 was methylated in 26 of 50 (52%) primary prostate cancers, but was not methylated in normal tissues or benign hyperplasias. Three of four tumors that metastasized, five of six that were poorly differentiated and all that were assigned a Gleason score higher than 8 (7/7) were methylated in the promoter of TIG1. The samples with peripheral invasion were more frequently methylated (21/32, 66%) than tissues without peripheral invasion (5/18, 28%). In addition, Gleason 7-10 cancers (21/30, 70%) were significantly more frequently methylated compared with Gleason 4-6 cancers (4/18, 22%) (Po0.01). The retinoic acid receptor beta (RAR-beta) gene was frequently methylated as well (42/50, 84%). When TIG1 showed methylation, RAR-beta was also methylated (25/26 samples). In almost all samples where RAR-beta was not methylated, TIG1 was also in an unmethylated state (14/15 samples). The methylation of TIG1 and RAR-beta was positively correlated (r ¼ 0.35; P ¼ 0.017). It is possible that the methylation of the retinoid response gene TIG1 occurred in response to the methylation and inactivation of RAR-beta. These observations may contribute to our understanding of mechanistic events leading to CpG island methylation in cancer.

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Section: Methylation Analysis Of the Er-beta And Rassf1a Promoter Regmentioning

confidence: 99%

Section: Expression Of Tig1mentioning

confidence: 99%

Section: Methylation Analysismentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Methylation of the retinoid response gene TIG1 in prostate cancer correlates with methylation of the retinoic acid receptor beta gene

2003

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“…Somatic mutational inactivation is rare in this gene (Dammann et al, 2000(Dammann et al, , 2003bAgathanggelou et al, 2001;Burbee et al, 2001;Lo et al, 2001). However, epigenetic inactivation of RASSF1A by hypermethylation of the promoter region has been described for a variety of human carcinomas including lung, breast, kidney, prostate, ovary, melanoma, gastric and nasopharyngeal carcinoma (Dammann et al, 2000Lerman and Minna, 2000;Agathanggelou et al, 2001;Byun et al, 2001;Lo et al, 2001;Yoon et al, 2001;Liu et al, 2002;Spugnardi et al, 2003). In addition, it is considered to be one of the most commonly methylated genes in human cancer.…”

Section: Introductionmentioning

confidence: 99%

Frequent hypermethylation of RASSF1A in early flat-type colorectal tumors

et al. 2004

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Flat colorectal tumors, characterized by high-grade dysplasia from early small flat mucosal lesions, exhibit a relatively aggressive clinical behavior and are known for their infrequent K-ras mutations. In this study, we investigated the methylation status of the RASSF1A promoter in association with 3p LOH and K-ras mutations in 48 flat colorectal tumors (39 early carcinomas and nine intramucosal high-grade dysplasias). RASSF1A hypermethylation was detected in 39 of 48 (81.3%) tumors and RASSF1A methylation was also detected in 19 of 39 (49%) normal colonic mucosal tissues. 3p21.3 LOH was detected in 20 of 42 (47.6%) cases, but RASSF1 methylation was detected in cases with LOH (14 cases) and retention of 3p21.3 (20 cases). K-ras mutations were detected in seven of 48 (14.6%) tumors and the concordant occurrence of K-ras mutation and RASSF1A methylation was detected in three of 48 cases (6.3%). Overall, there was a statistically significant mutually exclusive relationship between K-ras mutations and RASSF1A methylation. In conclusion, promoter hypermethylation of RASSF1A is a frequent event and may start early in the background normal mucosa in this tumor type. An alternative cascade of abnormalities in RAS transduction pathways may be responsible for the flat morphology and aggressive nature of flat colorectal neoplasms.

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DNA methylation patterns of RAR‐β2 and RASSF1A gene promoters in FNAB samples from Greek population with benign or malignant breast lesions

Kougioumtsidou

Vavoulidis

Nasioutziki

et al. 2020

Diagnostic Cytopathology

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Background Promoter hypermethylation is common in Breast Cancer (BC) with studies mainly in histological specimens showing frequent methylation of tumor suppressor genes (TSGs) compared with normal tissues. The aim of this study was to estimate the frequency of promoter methylation of RAR‐β2 and RASSF1A genes in breast FNAB material aiming to evaluate the methylation status of these two genes as biomarker for detecting BC in Greek population. Methods FNAB material from 104 patients was collected for cytological evaluation and epigenetic analysis. DNA was extracted and subjected to bisulfite conversion. A methylation‐specific PCR was carried out and the final products were separated with electrophoresis in 2% agarose gels. Results From 104 samples, RASSF1A hypermethylation was observed in 78 (75%) and RAR‐β2 hypermethylation in 64 (61.6%). 84% and 78% of the cases diagnosed with breast malignancy (n = 50) were methylated for RASSF1A and RAR‐β2, respectively. Methylated RASSF1A and RAR‐β2 were also detected in 88.3% and 76.5% in samples diagnosed as suspicious for malignancy (n = 17) and in 57.2% of samples diagnosed with atypia (n = 14). The Odds Ratio for breast malignancy was 4.545 in patients with RASSF1A hypermethylation and 9.167 in patients with RAR‐β2 hypermethylation underlying their promoter's methylation positive correlation with breast malignancy. Conclusion To optimize the sensitivity and specificity of this epigenetic setting, more TSGs related to BC should be gradually imported in our evaluated methylation panel and be validated in a larger study sample with the aim that the obtained epigenetic profiles will provide clinicians with valuable tools for management of BC patients in Greece.

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Frequent hypermethylation of the RASSF1A gene in prostate cancer

Cited by 145 publications

References 38 publications

Methylation of the retinoid response gene TIG1 in prostate cancer correlates with methylation of the retinoic acid receptor beta gene

Methylation of the retinoid response gene TIG1 in prostate cancer correlates with methylation of the retinoic acid receptor beta gene

Frequent hypermethylation of RASSF1A in early flat-type colorectal tumors

DNA methylation patterns of RAR‐β2 and RASSF1A gene promoters in FNAB samples from Greek population with benign or malignant breast lesions

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