A 5′-CG-3′-rich region in the promoter of the transcriptionally frequently silenced RET protooncogene lacks methylated cytidine residues

Munnes, M.; Patrone, Giovanna; Schmitz, Birgit; Romeo, Giovanni; Doerfler, Walter

doi:10.1038/sj.onc.1202165

Cited by 40 publications

(33 citation statements)

References 27 publications

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“…3). In a region of about 900 base pairs, 95 unmethylated 5Ј-CG-3Ј dinucleotides are located of which the majority lies within the putative promoter segment [Munnes et al, 1998]. During embryogenesis, RET proto-oncogene expression is regulated in a temporally and spatially defined pattern [Avantaggio et al, 1994;Schuchardt et al, 1995].…”

Section: Discussionmentioning

confidence: 99%

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Familial form of Hirschsprung disease: Nucleotide sequence studies reveal point mutations in the RET proto-oncogene in two of six families but not in other candidate genes

et al. 2000

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Hirschsprung disease (HSCR; McKusick 142623) or aganglionic megacolon is a frequent (1 in 5,000 live births) heritable disorder of the enteric nervous system. By haplotyping with a variety of microsatellite markers, by amplifying all 20 exons of the RET proto-oncogene and by applying a direct DNA sequencing protocol, we have analyzed the DNA from HSCR patients in 6 different families. In one family with a joint occurrence of HSCR and FMTC (follicular medullary thyroid carcinoma), we have identified a mutation in codon 609 in one out of 6 cysteine residues encoded in exon 10 of the RET gene. This C609R point mutation has not previously been reported to cause HSCR. In 2 of the HSCR patients described here from different families, we have found a mutation in exon 2 (R77C) and a silent mutation in exon 3 (Y204Y), respectively, in the extracellular part of the RET proto-oncogene. In introns 2 and 17 of the RET proto-oncogene in 2 families, we have detected single nucleotide exchanges that are probably polymorphisms with unknown, if any, relations to HSCR. The DNA sequences of 5 further genes (GDNF, GDNFRalpha, EDN3, EDNRB, and NTN), that may contribute to the development of HSCR, have not shown mutations in the patients analyzed so far. In 2 of the reported families with several affected children and one grandchild, sequence analyses revealed no mutations in the coding regions of any of the candidate genes analyzed.

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Section: Discussionmentioning

confidence: 99%

“…1, 3). sively in the substantia nigra, the adrenal medulla, cerebellum and other parts of the brain [Takaya et al, 1996;Munnes et al, 1998]. Tumor tissues like pheochromocytomas, medullary thyroid carcinomas (MTC) and papillary thyroid carcinomas (PTC) also harbor RET transcripts.…”

Section: Discussionmentioning

confidence: 99%

Familial form of Hirschsprung disease: Nucleotide sequence studies reveal point mutations in the RET proto-oncogene in two of six families but not in other candidate genes

et al. 2000

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“…Details of these methods as performed in this laboratory were described previously: Southern hybridization (Southern 1975;Koetsier et al 1993), PCR (Munnes et al 1998), fluorescent in situ hybridization (Heller et al 1995).…”

Section: Standard Molecular Biological Methodsmentioning

confidence: 99%

The gastrointestinal tract as the portal of entry for foreign macromolecules: fate of DNA and proteins

et al. 2003

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The gastrointestinal tract (GIT) of mammals is the main portal of entry for foreign DNA and proteins. We have documented the fate of orally administered DNA or protein in the GIT of the mouse. The gene for the Green Fluorescent Protein (GFP) (4.7 kb) and the genomes of bacteriophage M13 (7.25 kb) and adenovirus type 2 (Ad2; 35.9 kb) were used as test DNAs. Persistence of these DNAs in the GIT was monitored by Southern hybridization and fluorescent in situ hybridization (FISH) or by PCR. For studies on proteins, recombinant glutathione-S-transferase was fed to mice. Survival of the protein in the GIT was then assessed by Western blotting. Depending on feeding schedules and food regimens, but irrespective of mouse strain or DNA length, fragments of the GFP gene or other DNAs were detectable for up to 18 h after feeding by Southern blot analysis. The GFP DNA could be visualized by FISH in cecal epithelia. A high fiber diet reduced the time required for food to pass through the GIT, and foreign DNA was cleared more rapidly. A high fat diet or complexing of the foreign DNA with protamine or lipofectin did not extend DNA persistence times. Undegraded GST protein was detected only in foregut contents up to 30 min after feeding. At 15 and 30 min post feeding, trace amounts of GST were found in extracts of the kidney. The GIT is constantly exposed to highly recombinogenic fragments of foreign DNA and to intact foreign proteins. Our data have implications for studies on carcinogenesis and mutagenesis, and on the pathogenicity of infectious proteins such as prions.

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“…We investigated the level of DNA methylation in a DNA segment of about 1,000 bp in the promoter and 5 -upstream region of this gene (Munnes et al 1998). By again apply-ing the bisulfite genomic sequencing technique, DNA from peripheral white blood cells (PWBCs) from healthy individuals or from Hirschsprung disease patients was used as well as DNA from different human tissues and from a human embryonic kidney cell line.…”

Section: The Promoter and 5 -Upstream Region Of The Ret Protooncogenementioning

confidence: 99%

“…In in vitro experiments in which the transcriptional activity of the RET gene promoter was assessed in linkage to an indicator gene after transfection into human cells, the activity of this promoter was decreased by HpaII (5 -CCGG-3 ) methylation and abolished by SssI (5 -CG-3 ) methylation. Hence the RET protooncogene promoter is sensitive to DNA methylation at least in transfection and transient transcription experiments (Munnes et al 1998). …”

Section: The Promoter and 5 -Upstream Region Of The Ret Protooncogenementioning

confidence: 99%

De Novo Methylation, Long-Term Promoter Silencing, Methylation Patterns in the Human Genome, and Consequences of Foreign DNA Insertion

Doerfler

Current Topics in Microbiology and Immunology

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A 5′-CG-3′-rich region in the promoter of the transcriptionally frequently silenced RET protooncogene lacks methylated cytidine residues

Cited by 40 publications

References 27 publications

Familial form of Hirschsprung disease: Nucleotide sequence studies reveal point mutations in the RET proto-oncogene in two of six families but not in other candidate genes

Familial form of Hirschsprung disease: Nucleotide sequence studies reveal point mutations in the RET proto-oncogene in two of six families but not in other candidate genes

The gastrointestinal tract as the portal of entry for foreign macromolecules: fate of DNA and proteins

De Novo Methylation, Long-Term Promoter Silencing, Methylation Patterns in the Human Genome, and Consequences of Foreign DNA Insertion

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