Hypomethylation and hypermethylation of DNA in Wilms tumors

Ehrlich, Melanie; Jiang, Guanchao; Fiala, Emerich S.; Dome, Jeffrey S.; Yu, Mimi C.; Long, Theodore; Youn, Byungwoo; Sohn, Ock Soon; Widschwendter, Martin; Tomlinson, Gail E.; Chintagumpala, Murali; Champagne, Martin A.; Parham, David M.; Liang, Gangning; Malik, Karim; Laird, Peter W.

doi:10.1038/sj.onc.1205890

Cited by 163 publications

(135 citation statements)

References 32 publications

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“…We demonstrate hypermethylation of the MCJ intronic CpG island 16,17 26 and >50% of ovarian cancers; 16,17 however, MCJ hypermethylation has not been investigated in other tumour types. Our observations of MCJ hypermethylation in medulloblastomas, stPNETs and ependymomas suggest that MCJ inactivation plays a role in the development of a range of CNS tumour types, and this role now requires further investigation and clarification.…”

Section: Discussionmentioning

confidence: 74%

“…Tumourspecific methylation of MCJ has also been reported in Wilms' tumours; 26 however, this is in contrast to ovarian cancers, where MCJ methylation is also a feature of the normal ovarian epithelium. 17 Strathdee et al 17 reported that the MCJ CpG island is methylated and the gene is not expressed in cells of epithelial origin but is unmethylated and expressed in cells of lymphocytic or fibroblast origin.…”

Section: Discussionmentioning

confidence: 96%

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Epigenetic inactivation ofMCJ (DNAJD1) in malignant paediatric brain tumours

et al. 2006

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Newcastle upon Tyne, United Kingdom MCJ (DNAJD1) is a recently discovered member of the DNAJ protein family whose expression is controlled epigenetically by methylation of a CpG island located within the 5 0 transcribed region of its gene. Methylation-dependent transcriptional silencing of MCJ has been observed in ovarian cancers and associated with increased resistance to chemotherapeutic agents; however, its role in other cancer types has not been widely investigated. We examined the status of MCJ in intracranial primitive neuroectodermal tumours [PNETs, comprising cerebellar PNETs (medulloblastomas) and supratentorial PNETs (stPNETs)] and ependymomas, together representing the most common malignant brain tumours of childhood. Evidence of MCJ hypermethylation was found in all 3 tumour types [medulloblastomas, 3/9 (33%) cell lines, 2/28 (7%) primary tumours; stPNETs, 2/2 (100%) cell lines, 3/10 (30%) primary tumours; and ependymomas, 2/20 (10%) primary tumours] but not in nonneoplastic brain tissues (n 5 11), indicating that MCJ methylation is a tumour-specific event. In methylated cases, the distribution of methylated CpG sites across the CpG island could be broadly divided into 2 patterns: (i) extensive methylation of the majority of CpG sites across the island or (ii) limited methylation of individual CpG sites concentrated towards the 5 0 end of the island. Extensive methylation patterns were associated with the methylation-dependent transcriptional silencing of MCJ in medulloblastoma and stPNET cell lines. Further investigations of the mechanism of MCJ inactivation revealed that its loss could occur either through biallelic epigenetic methylation or by methylation in association with genetic loss of its second allele. These data indicate that epigenetic inactivation of MCJ may play a role in the development of a range of paediatric brain tumour types, and its role in disease pathogenesis and chemotherapeutic resistance should now be investigated further. ' 2005 Wiley-Liss, Inc.Key words: MCJ; DNAJD1; primitive neuroectodermal tumour; medulloblastoma; ependymoma; hypermethylation Medulloblastoma is a PNET which arises in the cerebellum and accounts for approximately 20% of childhood brain tumours. 1 stPNETs are histologically similar to medulloblastomas but arise in the cerebrum or pineal body and appear to exhibit different genetic aberrations. 2,3 Medulloblastomas and stPNETs are highly malignant, and overall 5-year survival rates following multimodal therapy are poor (approx. 60%). Current treatment regimes are also associated with long-term neurologic and endocrinologic side effects, and disease course is difficult to predict based on current clinical and pathologic indices. 1,4 Thus, a better understanding of the molecular events underlying the development of these tumours could provide the basis of an improved outlook for these patients, through identification of molecular markers for disease stratification and development of molecularly targeted therapeutic regimens.There has been significant inter...

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Section: Discussionmentioning

confidence: 74%

Section: Discussionmentioning

confidence: 96%

Epigenetic inactivation ofMCJ (DNAJD1) in malignant paediatric brain tumours

et al. 2006

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“…The overall m 5 C content of the DNA was determined by high performance liquid chromatography (HPLC) 24 on heat-denatured DNA digested with nuclease P1 and bacterial alkaline phosphatase for 2 h at 37˚C each.…”

Section: Methodsmentioning

confidence: 99%

“…Furthermore, we found, that a much higher percentage of Wilms tumors exhibited hypomethylation of Sat2 than pericentromeric rearrangements in Sat2 DNA-rich chromosomes as determined by karyotype analysis. 14 Because the high frequencies of cancer-linked satellite DNA hypomethylation are not positively associated with cancer-linked CpG island hypermethylation of tumor suppressor genes 8,24 (Laird P, Dubeau L, Ehrlich M, unpublished data), this hypomethylation is not likely to be just a byproduct of or preliminary to CpG island hypermethylation. These findings suggest that there are other ways by which cancer-linked satellite DNA hypomethylation contributes to oncogenesis besides favoring karyotypic instability, e.g., possibly by influencing gene expression in trans.…”

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confidence: 99%

DNA hypomethylation is prevalent even in low-grade breast cancers

Jackson¹,

Yu²,

Arakawa³

et al. 2004

Cancer Biology & Therapy

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109

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“…Hence, DNhpom agents might promote neoplasia in prospective tumour cells simultaneously with reactivation of HbF gene expression in erythrocytes precursors, residing inside the tumour tissues or in haematopoietic tissues of the same organism. This hypothesis is not impaired by the evidence for inactivation of tumour suppressing genes by DNA hypermethylation, since hypermethylation is specific for unique genomic sites while at the same time global DNA is hypomethylated (Ehrlich et al, 2002;Brothman et al, 2005;Ehrlich, 2005). By that ambiguity, the use of DNA demethylating agents as therapeutic anticancer regiment might contribute to carcinogenesis (Ehrlich, 2005).…”

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confidence: 99%

Foetal haemoglobin-blood cells (F-cells) as a feature of embryonic tumours (blastomas)

2007

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Tumour markers are important in the diagnosis and monitoring of many tumours. This study tested the hypothesis that an oncofoetal protein, foetal haemoglobin (HbF) is a potential tumour marker in embryonic tumours, useful for management. An immunohistochemical investigation of HbF blood cell (Fc) distribution was carried out in tumours and in bone marrow samples from 83 children and 13 adults with various embryonic tumours (blastomas), and in bone marrow samples of 24 leukaemia patients. In the three, main blastoma types, nephroblastoma (Wilms' tumour), neuroblastoma and retinoblastoma, where all the patients, except two, were children, around 80% of the tumour samples had Fc within proliferating blood vessels and spaces between tumour cells. In parallel, clusters of Fc, mostly F-erythroblasts (Feb), were distributed in the bone marrow of some of those patients and in the bone marrow of 79% of the leukaemia patients. Foetal haemoglobin, as well as being a potential prognostic cancer marker, is a potential indicator of DNA hypomethylation implicated in the development of these tumours, as well as in others previously noted for the presence of HbF.

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Hypomethylation and hypermethylation of DNA in Wilms tumors

Cited by 163 publications

References 32 publications

Epigenetic inactivation ofMCJ (DNAJD1) in malignant paediatric brain tumours

Epigenetic inactivation ofMCJ (DNAJD1) in malignant paediatric brain tumours

DNA hypomethylation is prevalent even in low-grade breast cancers

Foetal haemoglobin-blood cells (F-cells) as a feature of embryonic tumours (blastomas)

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