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Epigenetic silencing of the ANKRD26 gene correlates to the pro-inflammatory profile and increased cardio-metabolic risk factors in human obesity.

Authors :
Desiderio, Antonella
Longo, Michele
Parrillo, Luca
Campitelli, Michele
Cacace, Giuseppe
de Simone, Sonia
Spinelli, Rosa
Zatterale, Federica
Cabaro, Serena
Dolce, Pasquale
Formisano, Pietro
Milone, Marco
Miele, Claudia
Beguinot, Francesco
Raciti, Gregory A.
Source :
Clinical Epigenetics; 12/4/2019, Vol. 11 Issue 1, pN.PAG-N.PAG, 1p
Publication Year :
2019

Abstract

Background: Obesity is a major worldwide threat to human health. Increasing evidence indicates that epigenetic modifications have a major impact on the natural history of this disorder. Ankyrin Repeat Domain 26 (Ankrd26) is involved in the development of both obesity and diabetes in mice and is modulated by environmentally induced epigenetic modifications. This study aims at investigating whether impaired ANKRD26 gene expression and methylation occur in human obesity and whether they correlate to the phenotype of these subjects. Results: We found that downregulation of ANKRD26 mRNA and hyper-methylation of a specific region of the ANKRD26 promoter, embedding the CpG dinucleotides − 689, − 659, and − 651 bp, occur in peripheral blood leukocytes from obese compared with the lean subjects. ANKRD26 gene expression correlates inversely to the percentage of DNA methylation at these 3 CpG sites. Luciferase assays reveal a cause-effect relationship between DNA methylation at the 3 CpG sites and ANKRD26 gene expression. Finally, both ANKRD26 mRNA levels and CpG methylation correlate to body mass index and to the pro-inflammatory status and the increased cardio-metabolic risk factors of these same subjects. Conclusion: Downregulation of the ANKRD26 gene and hyper-methylation at specific CpGs of its promoter are common abnormalities in obese patients. These changes correlate to the pro-inflammatory profile and the cardio-metabolic risk factors of the obese individuals, indicating that, in humans, they mark adverse health outcomes. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
18687075
Volume :
11
Issue :
1
Database :
Complementary Index
Journal :
Clinical Epigenetics
Publication Type :
Academic Journal
Accession number :
140157547
Full Text :
https://doi.org/10.1186/s13148-019-0768-0