AI Article Synopsis
- Maternal prenatal psychosocial stress negatively impacts the hypothalamic-pituitary-adrenal axis function in infants, with unknown biological mechanisms possibly linked to altered DNA methylation.
- A study was conducted with 80 pregnant adolescents, measuring maternal distress via depression and anxiety, and assessing infant DNA methylation and cortisol levels at 12 months.
- Key findings indicated that elevated maternal anxiety and cortisol levels in late pregnancy were associated with lower DNA methylation of stress-related genes in infants, particularly the oxytocin receptor gene (OXTR), which may influence stress regulation.
Article Abstract
Maternal prenatal psychosocial stress is associated with adverse hypothalamic-pituitary-adrenal axis (HPAA) function among infants. Although the biological mechanisms influencing this process remain unknown, altered DNA methylation is considered to be one potential mechanism. We investigated associations between maternal prenatal psychological distress, infant salivary DNA methylation, and stress physiology at 12 months. Mother's distress was measured via depression and anxiety in early and late pregnancy in a cohort of 80 pregnant adolescents. Maternal hair cortisol was collected during pregnancy. Saliva samples were collected from infants at 12 months to quantify DNA methylation of three stress-related genes (FKBP5, NR3C1, OXTR) (n = 62) and diurnal cortisol (n = 29). Multivariable linear regression was used to test for associations between prenatal psychological distress, and infant DNA methylation and cortisol. Hair cortisol concentrations in late pregnancy were negatively associated with two sites of FKBP5 (site 1: B = -22.33, p = .003; site 2: B = -15.60, p = .012). Infants of mothers with elevated anxiety symptoms in late pregnancy had lower levels of OXTR2 CpG2 methylation (B = -2.17, p = .03) and higher evening salivary cortisol (B = 0.41, p = .03). Furthermore, OXTR2 methylation was inversely associated with evening cortisol (B = -0.14, p-value ≤ .001). Our results are, to our knowledge, the first evidence that the methylation of the oxytocin receptor may contribute to the regulation of HPAA during infancy.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9792831 | PMC |
| http://dx.doi.org/10.1002/dev.22352 | DOI Listing |
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