The association of psychological and trauma-related factors with biological and facial aging acceleration: evidence from the UK Biobank

The association of psychological and trauma-related factors with biological and facial aging acceleration: evidence from the UK Biobank

Psychological and trauma-related factors are associated with many diseases and mortality. However, a comprehensive assessment of the association between psycho-trauma exposures and aging acceleration is currently lacking. Using data from 332,359 UK Biobank participants, we calculated biological agin...

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Veröffentlicht in:BMC medicine 2024-09, Vol.22 (1), p.359-13, Article 359
Hauptverfasser: Wang, Junren, Han, Xin, Yang, Yao, Zeng, Yu, Qu, Yuanyuan, Yang, Huazhen, Song, Jie, Qiu, Changjian, Song, Huan
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Adverse Childhood Experiences
Age
Aged
Aging
Aging - physiology
Analysis
Anxiety
Biobanks
Biological aging acceleration
Biological effects
Biological Specimen Banks
Biomarkers
Care and treatment
Child & adolescent mental health
Children
Cluster analysis
Complications and side effects
Face
Facial aging acceleration
Female
Health aspects
Hospitals
Humans
Length of telomeres
Leukocytes
Likert scale
Male
Measurement
Mental depression
Mental disorders
Middle Aged
Mortality
Primary care
Psychic trauma
Psychological factors
Psychology, Pathological
Psychopathology
Regression analysis
Regression models
Telomeres
Trauma
Trauma experience
UK Biobank
United Kingdom
United Kingdom - epidemiology
Yeast
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Zusammenfassung:Psychological and trauma-related factors are associated with many diseases and mortality. However, a comprehensive assessment of the association between psycho-trauma exposures and aging acceleration is currently lacking. Using data from 332,359 UK Biobank participants, we calculated biological aging acceleration, indexed by the presence of leukocyte telomere length (LTL) deviation (i.e., the difference between genetically determined and observed LTL > 0). The acceleration of facial aging (i.e., looking older than the chronological age) was assessed using a self-report question. Then, we estimated the associations of each psycho-trauma factor with biological and facial aging acceleration, using logistic regression models adjusted for multiple important covariates. Furthermore, restricted to 99,180 participants with complete psychological and trauma-related data, we identified clusters of individuals with distinct psycho-trauma patterns using the latent class analysis method and assessed their associations with aging acceleration using similar models. We observed most of the studied psycho-trauma factors were associated with biological and facial aging acceleration. Compared to the "Absence of trauma and psychopathology" cluster, the "adverse childhood experiences (ACEs) with psychopathology" cluster showed strong associations with those aging measurements (odds ratio [OR] = 1.13 [1.05 - 1.23] for biological and 1.52 [1.18 - 1.95] for facial aging acceleration), while no such association was observed for the "ACEs without psychopathology" cluster (1.04 [0.99 - 1.09] and 1.02 [0.84 - 1.24]. Our study demonstrated significant associations of psycho-trauma factors with both biological and facial aging acceleration. The differential aging consequences observed among ACEs exposed individuals with and without psychopathology prompt interventions aimed to improve individuals' psychological resilience to prevent aging acceleration.
ISSN:1741-7015
1741-7015
DOI:10.1186/s12916-024-03578-7