DNA methylation GrimAge acceleration in US military veterans with PTSD

被引:0
|
作者
Seyma Katrinli
Anthony P. King
Elizabeth R. Duval
Alicia K. Smith
Nirmala Rajaram
Israel Liberzon
Sheila A. M. Rauch
机构
[1] Emory University,Department of Psychiatry & Behavioral Health, and Institute for Behavioral Medicine Research
[2] Department of Gynecology and Obstetrics,Department of Psychiatry
[3] The Ohio State University,Department of Psychiatry & Behavioral Science
[4] Michigan Medicine,undefined
[5] University of Michigan,undefined
[6] Emory University,undefined
[7] Department of Psychiatry & Behavioral Sciences,undefined
[8] Veterans Affairs Ann Arbor Healthcare System,undefined
[9] Texas A&M Health,undefined
[10] Atlanta VA Healthcare System GA,undefined
来源
Neuropsychopharmacology | 2023年 / 48卷
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摘要
Epigenetic alterations in DNA methylation might mediate gene expression effects of trauma underlying PTSD symptoms, or effects of PTSD on related health problems. PTSD is associated with all-cause morbidity and premature mortality, suggesting accelerated biological aging. We measured genome-wide DNA methylation (Illumina MethylationEPIC BeadChip) in whole blood in a treatment study for combat-related PTSD - “PROGrESS”, a multisite RCT comparing sertraline plus enhanced medication management (SERT + EMM), prolonged exposure (PE) therapy plus placebo (PE + PLB), and the combination (SERT + PE). DNA methylation was measured in 140 US military veterans who served in Iraq and/or Afghanistan (112 current PTSD cases enrolled in a PTSD treatment study and 28 veterans without PTSD history controls), and also 59 non-trauma exposed controls at baseline posttreatment (24 weeks after baseline). Increased DNA methylation GrimAge acceleration (p = 8.8e−09) was observed in patients with PTSD compared to a pooled control group (trauma exposed and non-trauma exposed), suggesting a higher risk of premature mortality in those with PTSD. There was no difference in GrimAge acceleration between combat trauma and non-trauma exposed controls. No treatment-related changes in GrimAge acceleration were found in within-subject comparisons of PTSD patients pre- to post-treatment.
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页码:773 / 780
页数:7
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