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Forkhead-box-O1 locus y marcadores metabólicos en los ancianos: estudio de asociación
Authors:Giulia Paroni  Filomena Addante  Davide Seripa  Francesco Panza  Massimiliano Copetti  Luigi Fontana  Alberto Pilotto
Institution:1. Unidad Geriátrica y Laboratorio de Investigación de Gerontología y Geriatría, Departamento de Ciencias Médicas, IRCCS Casa Sollievo della Sofferenza, San Giovanni Rotondo (FG), Italia;2. Unidad de Bioestadística, IRCCS Casa Sollievo della Sofferenza, San Giovanni Rotondo (FG), Italia;3. División de Nutrición y Envejecimiento, Instituto de Salud, Roma, Italia;4. Unidad Geriátrica, Empresa ULSS 16 Padua, Hospital San Antonio, Padua, Italia
Abstract:

Introduction

Mutations of forkhead-box-O1 (FOXO1) gene at locus 13q14.1 cause changes in biochemical parameters leading to premature aging. Protein FoxO1 participates in the regulation of biochemical pathways, including those influencing the regulation of lipid profile and glucose metabolism. These parameters are a risk factor for all-cause mortality in the elderly population. The aim of this study was to investigate the relationship between FOXO1 locus and metabolic-nutritional markers.

Material and methods

Single-nucleotide polymorphisms (SNP) rs2721069, rs4943794 and rs7981045 were determined in 594 hospitalized elderly (65-99 years), patients consecutively admitted to a geriatric ward, and tested the association of FOXO1 variants with biological markers by the analyses of co-variance (ANCOVA) and by Genotype Score Model statistic.

Results

The ANCOVA analysis, under different genetic models, revealed significant associations. In particular, assuming a dominant genetic model, a significant association with serum levels of fasting glucose was observed for rs2721069 (P = .034) and rs4943794 (P = .012). For rs4943794 a significant association assuming a free genetic model (P = .039) and an additive one (P = .012) was also observed. No significant relationship was observed between rs7981045 and the analyzed markers. The Genotype Score Model analysis confirmed a significant association between FOXO1 SNP and fasting glucose, taking the SNP rs2721069 and rs4943794 together (P = .048; β = 3.198).

Conclusions

Aging is a complex process, resulting from the interaction between several factors, including environmental and genetic ones. Our findings suggest that FOXO1 locus may influence blood glucose levels in hospitalized older patients, thus being one of the genetic factors contributing to healthy aging.
Keywords:FoxO1  Metabolismo  Marcadores metabó  licos  Envejecimiento
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