Frailty, sex, and poverty are associated with DNA damage and repair in frail, middle-aged urban adults

IF 3 3区 生物学 Q2 GENETICS & HEREDITY
Jessica T. Smith , Nicole Noren Hooten , Nicolle A. Mode , Alan B. Zonderman , Ngozi Ezike , Simran Kaushal , Michele K. Evans
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引用次数: 0

Abstract

Frailty is an age-related syndrome characterized by reduced recovery from stressors and increased risks of morbidity and mortality. Although frailty is usually studied in those over 65 years, our previous work showed that frailty is both present and a risk factor for premature mortality in midlife. We identified altered gene expression patterns and biological pathways associated with inflammation in frailty. Evidence suggests DNA oxidation damage related to inflammation accumulates with age, and that DNA repair capacity (DRC) declines with age and age-related conditions. We hypothesized that inter-individual differences in DNA oxidation damage and DRC are associated with frailty status and poverty level. Using the CometChip assay, we assessed baseline single-strand breaks and hydrogen peroxide (H2O2)-induced DNA oxidation damage and DRC in non-frail and frail middle-aged African American and White individuals with household incomes above and below poverty. Analysis of baseline single-strand breaks showed no associations with frailty, poverty, race, or sex. However, we identified an interaction between frailty and poverty in H2O2-induced DNA oxidation damage. We also identified interactions between sex and frailty as well as sex and poverty status with DRC. The social determinant of health, poverty, associates with DRC in men. Baseline DNA damage, H2O2-induced DNA damage as well as DRC were associated with serum cytokine levels. IL-10 levels were inversely associated with baseline DNA damage as well as H2O2-induced DNA damage, DRC was altered by IL-4 levels and sex, and by TNF-α levels in the context of sex and poverty status. This is the first evidence that DRC may be influenced by poverty status at midlife. Our data show that social determinants of health should be considered in examining biological pathways through which disparate age-related health outcomes become manifest.

在体弱多病的中年城市成年人中,脆弱、性别和贫困与DNA损伤和修复有关
虚弱是一种与年龄有关的综合征,其特点是从压力源中恢复能力降低,发病率和死亡率增加。虽然虚弱通常在65岁以上的人群中进行研究,但我们之前的工作表明,虚弱既是存在的,也是中年过早死亡的一个风险因素。我们确定了与虚弱炎症相关的基因表达模式和生物学途径的改变。有证据表明,与炎症相关的DNA氧化损伤随着年龄的增长而积累,DNA修复能力(DRC)随着年龄和年龄相关疾病的增长而下降。我们假设DNA氧化损伤和DRC的个体间差异与脆弱状态和贫困水平有关。使用CometChip分析,我们评估了非体弱和体弱中年非洲裔美国人和家庭收入在贫困线以上和贫困线以下的白人个体的基线单链断裂和过氧化氢(H2O2)诱导的DNA氧化损伤和DRC。基线单链断裂分析显示与虚弱、贫穷、种族或性别无关。然而,我们在h2o2诱导的DNA氧化损伤中发现了虚弱和贫穷之间的相互作用。我们还确定了性别与脆弱以及性别与刚果民主共和国贫困状况之间的相互作用。健康的社会决定因素贫困与男性的刚果民主共和国有关。基线DNA损伤、h2o2诱导的DNA损伤以及DRC与血清细胞因子水平相关。IL-10水平与基线DNA损伤和h2o2诱导的DNA损伤呈负相关,DRC受IL-4水平和性别的影响,在性别和贫困状况下受TNF-α水平的影响。这是刚果民主共和国可能受到中年贫困状况影响的第一个证据。我们的数据表明,在检查与年龄相关的不同健康结果变得明显的生物学途径时,应该考虑健康的社会决定因素。
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来源期刊
DNA Repair
DNA Repair 生物-毒理学
CiteScore
7.60
自引率
5.30%
发文量
91
审稿时长
59 days
期刊介绍: DNA Repair provides a forum for the comprehensive coverage of DNA repair and cellular responses to DNA damage. The journal publishes original observations on genetic, cellular, biochemical, structural and molecular aspects of DNA repair, mutagenesis, cell cycle regulation, apoptosis and other biological responses in cells exposed to genomic insult, as well as their relationship to human disease. DNA Repair publishes full-length research articles, brief reports on research, and reviews. The journal welcomes articles describing databases, methods and new technologies supporting research on DNA repair and responses to DNA damage. Letters to the Editor, hot topics and classics in DNA repair, historical reflections, book reviews and meeting reports also will be considered for publication.
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