Germline epimutation of MLH1 in individuals with multiple cancers

Suter, Catherine M.; Martin, David I. K.; Ward, Robyn L.

doi:10.1038/ng1342

Cited by 422 publications

(331 citation statements)

References 28 publications

(26 reference statements)

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“…No methylation was detected in their peripheral blood lymphocytes (data not shown), suggesting that methylation was somatically acquired and localized, as opposed to constitutional, such as that found in carriers of MLH1 epimutations. [34][35][36][37] In the tumours of each of these seven cases, at least one additional gene within 3p22 was concomitantly methylated with MLH1 ( Figure 6). In five cases, the tumours were BRAF V600E mutant and in four the tumours were CIMP þ (Table 6).…”

Section: Association Between Methylation Of Individual 3p22 Genes Rementioning

confidence: 98%

Methylation of the 3p22 region encompassing MLH1 is representative of the CpG island methylator phenotype in colorectal cancer

et al. 2011

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Epigenetic silencing of cancer-related genes by promoter methylation is a frequent event in sporadic colorectal cancer. The CpG island methylator phenotype (CIMP þ ), in which discrete genes throughout the genome are simultaneously methylated, and long-range epigenetic silencing, whereby multiple genes within contiguous chromosomal regions are methylated, have been described in subsets of colorectal cancer. We previously reported the concurrent methylation of the mismatch repair gene MLH1 with a cluster of flanking genes in chromosome region 3p22 in sporadic colorectal carcinoma exhibiting microsatellite instability and the BRAF V600E mutation. Herein, we aimed to determine whether methylation of MLH1 and neighbouring 3p22 genes, singly or concomitantly, correlate with the germline c.-93G4A SNP within the MLH1 promoter, CIMP þ and other clinicopathological and molecular features of the tumours. By studying a cohort of 946 sporadic colorectal cancer cases, we show a strong association between concordant methylation of Z3 of five 3p22 genes with CIMP þ and the BRAF V600E mutation (Po0.001). These associations were independent of microsatellite instability, as concomitant methylation of 3p22 genes other than MLH1 was found in microsatellite stable cancers. These findings show that long-range epigenetic silencing across 3p22 occurs in the context of CIMP þ and the BRAF V600E mutation, and only gives rise to microsatellite instability when this process encompasses MLH1. Furthermore, the strong relationship between long-range epigenetic silencing of 3p22 and CIMP þ provides further evidence that these two purportedly distinct epigenetic phenotypes represent a single entity with a common aetiology. Low-level methylation of MLH1 and flanking 3p22 genes, as well as the BRAF V600E mutation, were detected in the apparently normal colonic mucosa of a small number of cases whose tumours showed a similar molecular profile, suggesting that these concurring genetic and epigenetic events can occur as a field defect in neoplastic development.

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Section: Association Between Methylation Of Individual 3p22 Genes Rementioning

confidence: 98%

Methylation of the 3p22 region encompassing MLH1 is representative of the CpG island methylator phenotype in colorectal cancer

et al. 2011

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“…Hypermethylation of tumor suppressor genes is generally associated with transcriptional repression to give rise to reduced expression or even gene silencing. Furthermore, hypermethylation of tumor suppressor genes can be an early event in cancer development [29][30][31] suggesting that both epigenetic modifications and genetic mutations can contribute to the disfunction of tumor suppressor genes, leading ultimately to tumor formation.…”

Section: Dna Methyltransferases Tumor Suppressor Genes and Cancer Dementioning

confidence: 99%

Epigenetic changes in virus-associated human cancers

Leu

Chang

2005

Cell Res

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Epigenetics of human cancer becomes an area of emerging research direction due to a growing understanding of specific epigenetic pathways and rapid development of detection technologies. Aberrant promoter hypermethylation is a prevalent phenonmena in human cancers. Tumor suppressor genes are often hypermethylated due to the increased activity or deregulation of DNMTs. Increasing evidence also reveals that viral genes are one of the key players in regulating DNA methylation. In this review, we will focus on hypermethylation and tumor suppressor gene silencing and the signal pathways that are involved, particularly in cancers closely associated with the hepatitis B virus, simian virus 40 (SV40), and Epstein-Barr virus. In addition, we will discuss current technologies for genome-wide detection of epigenetically regulated targets, which allow for systematic DNA hypermethylation analysis. The study of epigenetic changes should provide a global view of gene profile in cancer, and epigenetic markers could be used for early detection, prognosis, and therapy of cancer.

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“…Patients with a tumour with MSI and somatic hypermethylation of the MLH1 promoter rarely carry a germline mutation in the MMR system, although rare exceptions have been reported. A few families have been described in which Lynch syndrome patients display hypermethylation of the MLH1 promoter in tumour as well as in non-tumour tissue (Gazzoli et al, 2002;Miyakura et al, 2004;Suter et al, 2004;Hitchins et al, 2005;Valle et al, 2007a). In addition, a family was recently described in which the susceptibility to tumours is caused by germline methylation of the MSH2 promoter (Chan et al, 2006).…”

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confidence: 99%

Patients with an unexplained microsatellite instable tumour have a low risk of familial cancer

et al. 2007

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The cancer risk is unknown for those families in which a microsatellite instable tumour is neither explained by MLH1 promoter methylation nor by a germline mutation in a mismatch repair (MMR) gene. Such information is essential for genetic counselling. Families suspected of Lynch syndrome (n ¼ 614) were analysed for microsatellite instability, MLH1 promoter methylation and/or germline mutations in MLH1, MSH2, MSH6, and PMS2. Characteristics of the 76 families with a germline mutation (24 MLH1, 2 PMS2, 32 MSH2, and 18 MSH6) were compared with those of 18 families with an unexplained microsatellite instable tumour. The mean age at diagnosis of the index patients in both groups was comparable at 44 years. Immunohistochemistry confirmed the loss of an MMR protein. Together this suggests germline inactivation of a known gene. The Amsterdam II criteria were fulfilled in 50/75 families (66%) that carried a germline mutation in an MMR gene and in only 2/18 families (11%) with an unexplained microsatellite instable tumour (Po0.0001). Current diagnostic strategies can detect almost all highly penetrant MMR gene mutations. Patients with an as yet unexplained microsatellite instable tumour likely carry a different type of mutation that confers a lower risk of cancer for relatives.

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Germline epimutation of MLH1 in individuals with multiple cancers

Cited by 422 publications

References 28 publications

Methylation of the 3p22 region encompassing MLH1 is representative of the CpG island methylator phenotype in colorectal cancer

Methylation of the 3p22 region encompassing MLH1 is representative of the CpG island methylator phenotype in colorectal cancer

Epigenetic changes in virus-associated human cancers

Patients with an unexplained microsatellite instable tumour have a low risk of familial cancer

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