DNA methylation in genes of longevity-regulating pathways: association wan obesity and metabolic complications

Salas-Pérez F.; Ramos-Lopez O.; Mansego M.L.; Milagro F.I.; Santos, J.L.; Riezu-Boj J.I.; Alfredo Martínez J.

Abstract

Aging is the main risk factor for most chronic diseases. Epigenetic mechanisms, such as DNA methylation (DNAm) plays a pivotal role in the regulation of physiological responses that can vary along lifespan. The aim of this research was to analyze the association between leukocyte DNAm in genes involved in longevity and the occurrence of obesity and related metabolic alterations in an adult population. Subjects from the MENA cohort (n=474) were categorized according to age (<45 vs 45>) and the presence of metabolic alterations: increased waist circumference, hypercholesterolemia, insulin resistance, and metabolic syndrome. The methylation levels of 58 CpG sites located at genes involved in longevity-regulating pathways were strongly correlated (FDRadjusted< 0.0001) with BMI. Fifteen of them were differentially methylated (p<0.05) between younger and older subjects that exhibited at least one metabolic alteration. Six of these CpG sites, located at MTOR (cg08862778), ULK1 (cg07199894), ADCY6 (cg11658986), IGF1R (cg01284192), CREB5 (cg11301281), and RELA (cg08128650), were common to the metabolic traits, and CREB5, RELA, and ULK1 were statistically associated with age. In summary, leukocyte DNAm levels of several CpG sites located at genes involved in longevity-regulating pathways were associated with obesity and metabolic syndrome traits, suggesting a role of DNAm in aging-related metabolic alterations.

Más información

Título según WOS: DNA methylation in genes of longevity-regulating pathways: association wan obesity and metabolic complications
Título según SCOPUS: DNA methylation in genes of longevity-regulating pathways: Association with obesity and metabolic complications
Título de la Revista: AGING-US
Volumen: 11
Número: 6
Editorial: IMPACT JOURNALS LLC
Fecha de publicación: 2019
Página de inicio: 1874
Página final: 1899
Idioma: English
DOI:

10.18632/aging.101882

Notas: ISI, SCOPUS