Your search keyword '"Fradin, Delphine"' showing total 3 results

1. CpG Methylation Changes within the IL2RA Promoter in Type 1 Diabetes of Childhood Onset.

Author

Belot, Marie-Pierre, Fradin, Delphine, Mai, Nga, Le Fur, Sophie, Zélénika, Diana, Kerr-Conte, Julie, Pattou, François, Lucas, Bruno, and Bougnères, Pierre

Subjects

*TYPE 1 diabetes, *PROMOTERS (Genetics), *DIABETES in children, *DNA methylation, *GENETIC polymorphisms, *SINGLE nucleotide polymorphisms

Abstract

None of the polymorphic variants of the IL2RA gene found associated with Type 1 Diabetes (T1D) was shown to have a functional effect. To test if the epigenetic variation could play a role at this locus, we studied the methylation of 6 CpGs located within the proximal promoter of IL2RA gene in 252 T1D patients compared with 286 age-matched controls. We found that DNA methylation at CpGs −373 and −456 was slightly but significantly higher in patients than in controls (40.4±4.6 vs 38.3±5.4, p = 1.4E4; 91.4±2.8 vs 89.5±5.3, p = 1.8E-6), while other CpG showed a strictly comparable methylation. Among 106 single nucleotide polymorphisms (SNPs) located in the neighboring 180kb region, we found that 28 SNPs were associated with DNA methylation at CpG −373. Sixteen of these SNPs were known to be associated with T1D. Our findings suggest that the effect of IL2RA risk alleles on T1D may be partially mediated through epigenetic changes. [ABSTRACT FROM AUTHOR]

Published

2013

2. Association of the CpG Methylation Pattern of the Proximal Insulin Gene Promoter with Type 1 Diabetes.

Author

Fradin, Delphine, Le Fur, Sophie, Mille, Clémence, Naoui, Nadia, Groves, Chris, Zelenika, Diana, McCarthy, Mark I., Lathrop, Mark, and Bougnè res, Pierre

Subjects

*METHYLATION, *ALKYLATION, *CHEMICAL reactions, *HYDROCARBONS, *INSULIN, *HORMONES, *GENES, *DIABETES

Abstract

The insulin (INS) region is the second most important locus associated with Type 1 Diabetes (T1D). The study of the DNA methylation pattern of the 7 CpGs proximal to the TSS in the INS gene promoter revealed that T1D patients have a lower level of methylation of CpG -19, -135 and -234 (p = 2.10-16) and a higher methylation of CpG -180 than controls, while methylation was comparable for CpG -69, -102, -206. The magnitude of the hypomethylation relative to a control population was 8-15% of the corresponding levels in controls and was correlated in CpGs -19 and -135 (r = 0.77) and CpG - 135 and -234 (r = 0.65). 70/485 (14%) of T1D patients had a simultaneous decrease in methylation of CpG -19, -135, -234 versus none in 317 controls. CpG methylation did not correlate with glycated hemoglobin or with T1D duration. The methylation of CpG -69, -102, -180, -206, but not CpG -19, -135, -234 was strongly influenced by the cis-genotype at rs689, a SNP known to show a strong association with T1D. We hypothesize that part of this genetic association could in fact be mediated at the statistical and functional level by the underlying changes in neighboring CpG methylation. Our observation of a CpG-specific, locus-specific methylation pattern, although it can provide an epigenetic biomarker of a multifactorial disease, does not indicate whether the reported epigenetic pattern preexists or follows the establishment of T1D. To explore the effect of chronic hyperglycemia on CpG methylation, we studied non obese patients with type 2 diabetes (T2D) who were found to have decreased CpG-19 methylation versus age-matched controls, similar to T1D (p = 2.10-6) but increased CpG-234 methylation (p = 5.10-8), the opposite of T1D. The causality and natural history of the different epigenetic changes associated with T1D or T2D remain to be determined. [ABSTRACT FROM AUTHOR]

Published

2012

3. Parent-Of-Origin Effects in Autism Identified through Genome-Wide Linkage Analysis of 16,000 SNPs.

Author

Fradin, Delphine, Cheslack-Postava, Keely, Ladd-Acosta, Christine, Newschaffer, Craig, Chakravarti, Aravinda, Arking, Dan E., Feinberg, Andrew, and Fallin, M. Daniele

Subjects

*AUTISM, *GENETICS, *GENOMES, *MENTAL health, *HEREDITY, *CELL nuclei, *GERMPLASM, *PATHOLOGICAL psychology, *DEVELOPMENTAL disabilities

Abstract

Background: Autism is a common heritable neurodevelopmental disorder with complex etiology. Several genome-wide linkage and association scans have been carried out to identify regions harboring genes related to autism or autism spectrum disorders, with mixed results. Given the overlap in autism features with genetic abnormalities known to be associated with imprinting, one possible reason for lack of consistency would be the influence of parent-of-origin effects that may mask the ability to detect linkage and association. Methods and Findings: We have performed a genome-wide linkage scan that accounts for potential parent-of-origin effects using 16,311 SNPs among families from the Autism Genetic Resource Exchange (AGRE) and the National Institute of Mental Health (NIMH) autism repository. We report parametric (GH, Genehunter) and allele-sharing linkage (Aspex) results using a broad spectrum disorder case definition. Paternal-origin genome-wide statistically significant linkage was observed on chromosomes 4 (LODGH = 3.79, empirical p<0.005 and LODAspex = 2.96, p = 0.008), 15 (LODGH = 3.09, empirical p<0.005 and LODAspex = 3.62, empirical p = 0.003) and 20 (LODGH = 3.36, empirical p<0.005 and LODAspex = 3.38, empirical p = 0.006). Conclusions: These regions may harbor imprinted sites associated with the development of autism and offer fruitful domains for molecular investigation into the role of epigenetic mechanisms in autism. [ABSTRACT FROM AUTHOR]

Published

2010