在一个多种族/民族的老年人样本中,抑郁症状部分介导了社会心理因素与表观遗传年龄加速之间的关系

IF 3.7 Q2 IMMUNOLOGY
Lauren A. Opsasnick , Wei Zhao , Lauren L. Schmitz , Scott M. Ratliff , Jessica D. Faul , Xiang Zhou , Belinda L. Needham , Jennifer A. Smith
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引用次数: 0

摘要

社会心理因素,包括累积的社会心理压力和孤独,与老年人的表观遗传衰老有关。此外,抑郁症状与社会心理因素和表观遗传衰老都有关系。然而,尚不清楚抑郁症状是否介导社会心理因素与表观遗传衰老之间的关联。我们对来自健康与退休研究的2681名老年人(平均年龄:70.4岁)的多种族/民族样本进行了线性回归模型,以检验社会心理压力、孤独和抑郁症状与DNA甲基化估计的五种表观遗传年龄加速(AA)指标之间的关系。对于所有确定的关联,我们测试了性别和受教育程度对效果的影响,并进行了中介分析,以表征抑郁症状在这些关联中的作用。心理社会压力、孤独感和抑郁症状均与至少一种表观遗传AA相关(FDR q <;0.05)。此外,我们观察到孤独、社会心理压力和性别在DunedinPACE上的相互作用,以及孤独和教育程度在GrimAA、PhenoAA和DunedinPACE上的相互作用,女性和没有大学学历的个体对表观遗传衰老的社会心理影响更为敏感。抑郁症状在心理社会压力与HannumAA、GrimAA和DunedinPACE之间的关系中分别起到24%至35%的中介作用,在孤独与GrimAA和DunedinPACE之间的关系中分别起到40%和37%的中介作用。本研究结果可能有助于阐明社会心理因素与表观遗传衰老之间的关系,这对于理解社会心理因素可能导致年龄相关疾病的生物学机制至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Depressive symptoms partially mediate the relationship between psychosocial factors and epigenetic age acceleration in a multi-racial/ethnic sample of older adults
Psychosocial factors, including cumulative psychosocial stress and loneliness, have been linked to epigenetic aging in older adults. Further, depressive symptoms have established relationships with both psychosocial factors and epigenetic aging. However, it is not known whether depressive symptoms mediate the association between psychosocial factors and epigenetic aging.
We conducted linear regression models to examine associations between psychosocial stress, loneliness, and depressive symptoms and five epigenetic age acceleration (AA) measures estimated by DNA methylation in a multi-racial/ethnic sample of 2681 older adults from the Health and Retirement Study (mean age: 70.4 years). For all identified associations, we tested for effect modification by sex and educational attainment and performed mediation analysis to characterize the role of depressive symptoms on these associations.
Psychosocial stress, loneliness, and depressive symptoms were each associated with at least one measure of epigenetic AA (FDR q < 0.05). Further, we observed interactions between loneliness, psychosocial stress, and sex on DunedinPACE, as well as loneliness and educational attainment on GrimAA, PhenoAA, and DunedinPACE, with females and individuals without a college degree appearing more sensitive to the psychosocial effects on epigenetic aging. Depressive symptoms mediated between 24 % and 35 % of the relationships between psychosocial stress and HannumAA, GrimAA, and DunedinPACE, as well as 40 % and 37 % of the relationships between loneliness and both GrimAA and DunedinPACE, respectively.

Results

from this study may help elucidate the relationship between psychosocial factors and epigenetic aging, which is critical in understanding the biological mechanisms through which psychosocial factors may contribute to age-related disease.
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来源期刊
Brain, behavior, & immunity - health
Brain, behavior, & immunity - health Biological Psychiatry, Behavioral Neuroscience
CiteScore
8.50
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审稿时长
97 days
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