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Transl Psychiatry. 2023 Feb 27;13(1):72. doi: 10.1038/s41398-023-02370-0.
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Associations between epigenetic aging and childhood peer victimization, depression, and suicidal ideation in adolescence and adulthood: A study of two population-based samples.表观遗传衰老与儿童期同伴受害、青少年及成年期抑郁和自杀意念之间的关联:基于两个群体样本的研究
Front Cell Dev Biol. 2023 Jan 12;10:1051556. doi: 10.3389/fcell.2022.1051556. eCollection 2022.
3
Epigenome-wide DNA methylation analysis of whole blood cells derived from patients with GAD and OCD in the Chinese Han population.中国汉族人群中广泛性焦虑障碍和强迫症患者全血细胞来源的全基因组 DNA 甲基化分析。
Transl Psychiatry. 2022 Nov 7;12(1):465. doi: 10.1038/s41398-022-02236-x.
4
Promoting Racial/Ethnic Equity in Psychosocial Treatment Outcomes for Child and Adolescent Anxiety and Depression.促进儿童和青少年焦虑与抑郁心理社会治疗结果中的种族/民族公平性。
Psychiatr Res Clin Pract. 2022 Sep 9;4(3):80-88. doi: 10.1176/appi.prcp.20210044. eCollection 2022 Fall.
5
DNA methylation signatures of childhood trauma predict psychiatric disorders and other adverse outcomes 17 years after exposure.童年创伤的 DNA 甲基化特征可预测创伤暴露 17 年后出现的精神障碍和其他不良后果。
Mol Psychiatry. 2022 Aug;27(8):3367-3373. doi: 10.1038/s41380-022-01597-5. Epub 2022 May 11.
6
Five-Year Trends in US Children's Health and Well-being, 2016-2020.2016-2020 年美国儿童健康和福利的五年趋势
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The pediatric buccal epigenetic clock identifies significant ageing acceleration in children with internalizing disorder and maltreatment exposure.儿科口腔表观遗传时钟揭示了内化障碍和遭受虐待儿童的显著衰老加速现象。
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8
Telomere length and epigenetic age acceleration in adolescents with anxiety disorders.青少年焦虑障碍与端粒长度和表观遗传年龄加速。
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"GrimAge," an epigenetic predictor of mortality, is accelerated in major depressive disorder.“衰老时钟”(GrimAge)是死亡率的一个表观遗传预测指标,在重度抑郁症中加速。
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Persistence and course of mental health problems from childhood into adolescence: results of a 10-year longitudinal study.从儿童期到青春期心理健康问题的持续和进程:一项 10 年纵向研究的结果。
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儿童和青少年时期的抑郁和焦虑症状与表观遗传衰老的关联。

Associations of depression and anxiety symptoms in childhood and adolescence with epigenetic aging.

作者信息

Ingram Sarah J, Vazquez Alexandra Y, Klump Kelly L, Hyde Luke W, Burt S Alexandra, Clark Shaunna L

机构信息

Interdisciplinary Graduate Program in Genetics, Department of Psychiatry & Behavioral Sciences, Texas A&M University, United States of America.

Department of Psychology, Michigan State University, United States of America.

出版信息

J Affect Disord. 2024 May 1;352:250-258. doi: 10.1016/j.jad.2024.02.044. Epub 2024 Feb 13.

DOI:10.1016/j.jad.2024.02.044
PMID:38360371
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11000694/
Abstract

BACKGROUND

Childhood anxiety and depression symptoms are potential risk factors for accelerated biological aging. In child and adolescent twins, we tested whether these symptoms were associated with DNA methylation (DNAm) aging, a measure of biological aging.

METHODS

276 twins (135 pairs, 6 singletons) had DNAm assayed from saliva in middle childhood (mean = 7.8 years). Residuals of five different DNAm age estimates regressed on chronological age were used to indicate accelerated aging. Anxiety and depression symptoms were assessed in middle childhood and early adolescence using the Child Behavior Checklist. Mixed effect regression was used to examine potential relationships between anxiety or depression symptoms, and accelerated DNAm age. MZ twin difference analysis was then utilized to determine if associations were environmentally-driven or due to genetic or shared-environment confounding.

RESULTS

Anxiety and depression symptoms were not associated with accelerated DNAm aging in middle childhood. In early adolescence, only the Wu clock was significant and indicated that each one symptom increase in anxiety symptoms had an associated age acceleration of 0.03 years (~0.4 months; p = 0.019). MZ twin difference analysis revealed non-significant within-pair effects, suggesting genetic and shared environmental influences.

LIMITATIONS

Sample is predominantly male and white. Generalizability to other populations may be limited.

CONCLUSION

Accelerated DNAm aging of the Wu clock in middle childhood is associated with anxiety, but not depression, symptoms in early adolescence. Further, this association may be the result of shared genetic and environmental influences. Accelerated DNAm aging may serve as an early risk factor or predictor of later anxiety symptoms.

摘要

背景

儿童期焦虑和抑郁症状是生物衰老加速的潜在风险因素。在儿童和青少年双胞胎中,我们测试了这些症状是否与DNA甲基化(DNAm)衰老相关,DNAm衰老是一种生物衰老的测量指标。

方法

276名双胞胎(135对,6名单胎)在儿童中期(平均年龄 = 7.8岁)时进行了唾液DNAm检测。将五个不同的DNAm年龄估计值相对于实际年龄的残差用于表示衰老加速。使用儿童行为量表在儿童中期和青春期早期评估焦虑和抑郁症状。采用混合效应回归分析来检验焦虑或抑郁症状与DNAm衰老加速之间的潜在关系。然后利用同卵双胞胎差异分析来确定这种关联是由环境驱动的,还是由于基因或共享环境的混杂因素导致的。

结果

在儿童中期,焦虑和抑郁症状与DNAm衰老加速无关。在青春期早期,只有Wu时钟模型具有显著意义,表明焦虑症状每增加一个单位,年龄加速约0.03岁(约0.4个月;p = 0.019)。同卵双胞胎差异分析显示配对内效应不显著,表明存在基因和共享环境的影响。

局限性

样本主要为男性和白人。对其他人群的普遍性可能有限。

结论

儿童中期Wu时钟的DNAm衰老加速与青春期早期的焦虑症状相关,但与抑郁症状无关。此外,这种关联可能是基因和环境共同影响的结果。DNAm衰老加速可能是后期焦虑症状的早期风险因素或预测指标。