Your search keyword '"El-Maarri, Osman"' showing total 7 results

1. Association of COMT genotypes with S-COMT promoter methylation in growth-discordant monozygotic twins and healthy adults

Author

Schreiner Felix, El-Maarri Osman, Gohlke Bettina, Stutte Sonja, Nuesgen Nicole, Mattheisen Manuel, Fimmers Rolf, Bartmann Peter, Oldenburg Johannes, and Woelfle Joachim

Subjects

Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Catechol-O-Methyltransferase (COMT) plays a key role in dopamine and estrogen metabolism. Recently, COMT haplotypes rather than the single polymorphism Val158Met have been reported to underlie differences in protein expression by modulating mRNA secondary structure. So far, studies investigating the epigenetic variability of the S-COMT (soluble COMT) promoter region mainly focused on phenotypical aspects, and results have been controversial. Methods We assessed S-COMT promoter methylation in saliva and blood derived DNA with regard to early pre- and postnatal growth as well as to genotype for polymorphisms rs6269, rs4633, and rs4680 (Val158Met) in 20 monozygotic twin pairs (mean age 4 years), who were discordant for intrauterine development due to severe feto-fetal-transfusion syndrome. Methylation levels of two previously reported partially methylated cytosines were determined by the quantitative SIRPH (SNuPE- IP RP HPLC) assay. Results Overall, we observed a high variability of S-COMT promoter methylation, which did not correlate with individual differences in the pre- or postnatal growth pattern. Within the twin pairs however we noted a distinct similarity that could be linked to underlying COMT genotypes. This association was subsequently confirmed in a cohort of 93 unrelated adult controls. Interestingly, 158Val-alleles were found at both ends of the epigenotypical range, which is in accordance with a recently proposed model of COMT haplotypes corresponding to a continuum of phenotypical variability. Conclusion The strong heritable component of S-COMT promoter methylation found in our study needs to be considered in future approaches that focus on interactions between COMT epigenotype and phenotype.

Published

2011

2. Gender specific differences in levels of DNA methylation at selected loci from human total blood: a tendency toward higher methylation levels in males.

Author

El-Maarri, Osman, Becker, Tim, Junen, Judith, Manzoor, Syed, Diaz-Lacava, Amalia, Schwaab, Rainer, Wienker, Thomas, and Oldenburg, Johannes

Subjects

*METHYLATION, *TRANSMETHYLATION, *DNA, *GENETICS, *SEX chromosomes

Abstract

Abnormal patterns of DNA methylation are observed in many diseases such as tumors and imprinting disorders. Little is known about inter-individual and gender specific variations. Here, we report on accurate and sensitive quantitative measurements of methylation in DNA from total blood in 96 healthy human males and 96 healthy human females. Global methylation was estimated by studying two repetitive DNA elements, namely Line-1 and Alu repeats, while single loci were investigated for three differentially methylated regions (DMRs) at PEG3, NESP55 and H19 imprinted genes and two additional loci at Xq28 ( F8 gene) and at 19q13.4 (locus between PEG3 and ubiquitin specific protease 29). We observed inter-individual correlations in the degree of methylation between Alu and Line-1 repeats. Moreover, all studied CpGs showed slightly higher methylation in males ( P < 0.0003–0.0381), with the exception of DMRs at imprinted genes ( P = 0.0342–0.9616) which were almost equally methylated in both sexes with only a small tendency towards higher methylation in males. This observed difference could be due to the process of X chromosome inactivation or merely to the presence of an additional X chromosome in female cells or could be a result of downstream effects of sex determination. [ABSTRACT FROM AUTHOR]

Published

2007

3. Familial molar tissues due to mutations in the inflammatory gene, NALP7, have normal postzygotic DNA methylation.

Author

Djuric, Ugljesa, El-Maarri, Osman, Lamb, Barbara, Kuick, Rork, Seoud, Muheiddine, Coullin, Philippe, Oldenburg, Johannes, Hanash, Samir, and Slim, Rima

Subjects

*FAMILIAL diseases, *GENETIC disorders, *TISSUES, *GENETIC mutation, *HISTOLOGY, *GENETICS, *DISEASES

Abstract

An imprinting disorder has been believed to underlie the etiology of familial biparental hydatidiform moles (HMs) based on the abnormal methylation or expression of imprinted genes in molar tissues. However, the extent of the epigenetic defect in these tissues and the developmental stage at which the disorder begins have been poorly defined. In this study, we assessed the extent of abnormal DNA methylation in two HMs caused by mutations in the recently identified 19q13.4 gene, NALP7. We demonstrate normal postzygotic DNA methylation patterns at major repetitive and long interspersed nuclear elements (LINEs), genes on the inactive X-chromosome, three-cancer related genes, and CpG rich regions surrounding the PEG3 differentially methylated region (DMR). Our data provide a comprehensive assessment of DNA methylation in familial molar tissues and indicate that abnormal DNA methylation in these tissues is restricted to imprinted DMRs. The known role of NALP7 in apoptosis and inflammation pinpoints previously unrecognized pathways that could directly or indirectly underlie the abnormal methylation of imprinted genes in molar tissues. [ABSTRACT FROM AUTHOR]

Published

2006

4. Epigenetic control of the angiotensin-converting enzyme in endothelial cells during inflammation

Author

Mudersbach, Thomas, Siuda, Daniel, Kohlstedt, Karin, Fleming, Ingrid, and El-Maarri, Osman

Subjects

Epigenomics, Cell biology, Inflammatory Diseases, Immune Cells, Science, Immunology, Peptidyl-Dipeptidase A, Biochemistry, Epithelium, Enzyme Regulation, White Blood Cells, Animal Cells, DNA-binding proteins, Genetics, Medicine and Health Sciences, Humans, Gene Regulation, ddc:610, Enzyme Chemistry, Promoter Regions, Genetic, Cells, Cultured, Inflammation, DNA methylation, Blood Cells, Biology and life sciences, Tumor Necrosis Factor-alpha, Macrophages, Endothelial Cells, Proteins, Epithelial Cells, DNA, Chromatin, Regulatory Proteins, Nucleic acids, Biological Tissue, Gene Expression Regulation, Enzymology, Medicine, Epigenetics, Gene expression, Cellular Types, Anatomy, DNA modification, Chromatin modification, Research Article, Chromosome biology, Transcription Factors

Abstract

The angiotensin-converting enzyme (ACE) plays a central role in the renin-angiotensin system, which is involved in the regulation of blood pressure. Alterations in ACE expression or activity are associated with various pathological phenotypes, particularly cardiovascular diseases. In human endothelial cells, ACE was shown to be negatively regulated by tumor necrosis factor (TNF) α. To examine, whether or not, epigenetic factors were involved in ACE expression regulation, methylated DNA immunoprecipitation and RNA interference experiments directed against regulators of DNA methylation homeostasis i.e., DNA methyltransferases (DNMTs) and ten-eleven translocation methylcytosine dioxygenases (TETs), were performed. TNFα stimulation enhanced DNA methylation in two distinct regions within the ACE promoter via a mechanism linked to DNMT3a and DNMT3b, but not to DNMT1. At the same time, TET1 protein expression was downregulated. In addition, DNA methylation decreased the binding affinity of the transcription factor MYC associated factor X to the ACE promoter. In conclusion, DNA methylation determines the TNFα-dependent regulation of ACE gene transcription and thus protein expression in human endothelial cells.

Published

2019

5. DNA-Methylation Patterns in Trisomy 21 Using Cells from Monozygotic Twins

Author

M. Reza Sailani, Corinne Gehrig, Audrey Letourneau, Christelle Borel, Michel Guipponi, Anne Vannier, Stylianos E. Antonarakis, Youssef Hibaoui, Anis Feki, Ximena Bonilla, Federico Santoni, Dean Nizetic, Konstantin Popadin, Periklis Makrythanasis, Frederique Carre-Pigeon, El-Maarri, Osman, and Lee Kong Chian School of Medicine (LKCMedicine)

Subjects

Twins, lcsh:Medicine, Biology, DNA methyltransferase, Epigenesis, Genetic, Histones, 03 medical and health sciences, 0302 clinical medicine, Morphogenesis, Homeobox, Humans, ddc:576.5, Epigenetics, Promoter Regions, Genetic, lcsh:Science, 030304 developmental biology, Gene Library, Genetics, 0303 health sciences, DNA methylation, Multidisciplinary, lcsh:R, Methylation, Twins, Monozygotic, DNA Methylation, Fibroblasts, CpG Islands, Down Syndrome/*genetics/metabolism, Gene Expression Regulation, Histones/metabolism, Phenotype, Molecular biology, Chromosome 21, Induced pluripotent stem cells, DNA demethylation, Embryonic organ morphogenesis, Reduced representation bisulfite sequencing, lcsh:Q, Down Syndrome, 030217 neurology & neurosurgery, Research Article

Abstract

DNA methylation is essential in mammalian development. We have hypothesized that methylation differences induced by trisomy 21 (T21) contribute to the phenotypic characteristics and heterogeneity in Down syndrome (DS). In order to determine the methylation differences in T21 without interference of the interindividual genomic variation, we have used fetal skin fibroblasts from monozygotic (MZ) twins discordant for T21. We also used skin fibroblasts from MZ twins concordant for T21, normal MZ twins without T21, and unrelated normal and T21 individuals. Reduced Representation Bisulfite Sequencing (RRBS) revealed 35 differentially methylated promoter regions (DMRs) (Absolute methylation differences = 25%, FDR < 0.001) in MZ twins discordant for T21 that have also been observed in comparison between unrelated normal and T21 individuals. The identified DMRs are enriched for genes involved in embryonic organ morphogenesis (FDR = 1.60 e -03) and include genes of the HOXB and HOXD clusters. These DMRs are maintained in iPS cells generated from this twin pair and are correlated with the gene expression changes. We have also observed an increase in DNA methylation level in the T21 methylome compared to the normal euploid methylome. This observation is concordant with the up regulation of DNA methyltransferase enzymes (DNMT3B and DNMT3L) and down regulation of DNA demethylation enzymes (TET2 and TET3) observed in the iPSC of the T21 versus normal twin. Altogether, the results of this study highlight the epigenetic effects of the extra chromosome 21 in T21 on loci outside of this chromosome that are relevant to DS associated phenotypes. Published version

Published

2015

6. Methylation defect in imprinted genes detected in patients with an Albright's hereditary osteodystrophy like phenotype and platelet Gs hypofunction

Author

Christine Wittevrongel, Benedetta Izzi, Chantal Thys, Koenraad Devriendt, Francis de Zegher, Eric Legius, Kathleen Freson, Annick Van den Bruel, Diether Lambrechts, Inge Francois, Chris Van Geet, Veerle Labarque, Marc D'Hooghe, and El-Maarri, Osman

Subjects

Genomic imprinting, GRB10 Adaptor Protein, lcsh:Medicine, Pediatrics, Molecular Cell Biology, GTP-Binding Protein alpha Subunits, Gs, Membrane Receptor Signaling, Growth Retardation, lcsh:Science, Albright's hereditary osteodystrophy, Multidisciplinary, biology, Nuclear Proteins, Methylation, Signaling in Selected Disciplines, Hormone Receptor Signaling, Phenotype, Pseudohypoparathyroidism, DNA methylation, Medicine, Epigenetics, DNA modification, Research Article, Signal Transduction, musculoskeletal diseases, medicine.medical_specialty, Fibrous Dysplasia, Polyostotic, Insulin-Like Growth Factor II, Internal medicine, Chromogranins, Genetics, medicine, GNAS complex locus, Humans, natural sciences, Biology, Disorders of Imprinting, lcsh:R, Human Genetics, DNA Methylation, medicine.disease, Endocrinology, Genetics of Disease, Cancer research, biology.protein, Pseudopseudohypoparathyroidism, lcsh:Q, Endocrinological Signaling

Abstract

Background Pseudohypoparathyroidism (PHP) indicates a group of heterogeneous disorders whose common feature is represented by impaired signaling of hormones that activate Gsalpha, encoded by the imprinted GNAS gene. PHP-Ib patients have isolated Parathormone (PTH) resistance and GNAS epigenetic defects while PHP-Ia cases present with hormone resistance and characteristic features jointly termed as Albright's Hereditary Osteodystrophy (AHO) due to maternally inherited GNAS mutations or similar epigenetic defects as found for PHP-Ib. Pseudopseudohypoparathyroidism (PPHP) patients with an AHO phenotype and no hormone resistance and progressive osseous heteroplasia (POH) cases have inactivating paternally inherited GNAS mutations. Methodology/Principal Findings We here describe 17 subjects with an AHO-like phenotype that could be compatible with having PPHP but none of them carried Gsalpha mutations. Functional platelet studies however showed an obvious Gs hypofunction in the 13 patients that were available for testing. Methylation for the three differentially methylated GNAS regions was quantified via the Sequenom EpiTYPER. Patients showed significant hypermethylation of the XL amplicon compared to controls (36±3 vs. 29±3%; p

Published

2012

7. A genetic signature of spina bifida risk from pathway-informed comprehensive gene-variant analysis

Author

Thomas J. Hoffmann, Anna Lipzen, Jasper Rine, Jason Stein, Nicholas J. Marini, Suzan L. Carmichael, Crystal Wright, Edward J. Lammer, John S. Witte, Dennis A. Gilbert, Katherine D. Lazaruk, Jill Hardin, Gary M. Shaw, Len A. Pennacchio, and El-Maarri, Osman

Subjects

Spina Bifida, Anatomy and Physiology, lcsh:Medicine, Genetic Networks, medicine.disease_cause, Risk Factors, Models, 2.1 Biological and endogenous factors, Aetiology, lcsh:Science, Spinal Dysraphism, Homocysteine, Genetics, Pediatric, 0303 health sciences, education.field_of_study, Mutation, Multidisciplinary, 030305 genetics & heredity, Genomics, Hispanic or Latino, Medicine, Hispanic Americans, Metabolic Networks and Pathways, Research Article, Clinical Research Design, General Science & Technology, Population, European Continental Ancestry Group, Context (language use), Biology, White People, Neurological System, 03 medical and health sciences, Folic Acid, Rare Diseases, Genetic, Genome Analysis Tools, Clinical Research, medicine, Humans, Genetic Predisposition to Disease, Allele, education, Gene, Alleles, 030304 developmental biology, Genetic association, Nutrition, Models, Genetic, Whites, Gene Expression Profiling, Prevention, lcsh:R, Infant, Newborn, Case-control study, Neurosciences, Infant, Human Genetics, Newborn, Gene expression profiling, Neuroanatomy, Purines, Case-Control Studies, Genetics of Disease, Congenital Structural Anomalies, lcsh:Q

Abstract

Despite compelling epidemiological evidence that folic acid supplements reduce the frequency of neural tube defects (NTDs) in newborns, common variant association studies with folate metabolism genes have failed to explain the majority of NTD risk. The contribution of rare alleles as well as genetic interactions within the folate pathway have not been extensively studied in the context of NTDs. Thus, we sequenced the exons in 31 folate-related genes in a 480-member NTD case-control population to identify the full spectrum of allelic variation and determine whether rare alleles or obvious genetic interactions within this pathway affect NTD risk. We constructed a pathway model, predetermined independent of the data, which grouped genes into coherent sets reflecting the distinct metabolic compartments in the folate/one-carbon pathway (purine synthesis, pyrimidine synthesis, and homocysteine recycling to methionine). By integrating multiple variants based on these groupings, we uncovered two provocative, complex genetic risk signatures. Interestingly, these signatures differed by race/ethnicity: a Hispanic risk profile pointed to alterations in purine biosynthesis, whereas that in non-Hispanic whites implicated homocysteine metabolism. In contrast, parallel analyses that focused on individual alleles, or individual genes, as the units by which to assign risk revealed no compelling associations. These results suggest that the ability to layer pathway relationships onto clinical variant data can be uniquely informative for identifying genetic risk as well as for generating mechanistic hypotheses. Furthermore, the identification of ethnic-specific risk signatures for spina bifida resonated with epidemiological data suggesting that the underlying pathogenesis may differ between Hispanic and non-Hispanic groups.

Published

2011