Adolescent girls at familial risk for depression with more advanced adrenarche have altered gut microbiota
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Objectives
Rates of adolescent depression are rising, especially among girls, with children of depressed parents facing a three times higher risk. Emerging evidence suggests a link between gut microbiota, neural function, and depression risk, possibly through pathways that involve brain-body interactions, including the vagus nerve. During adolescence, sex-specific changes in the microbiota align with pubertal development, although their connection to depression vulnerability remains unclear. We compared gut microbiota in adolescents at high and low familial risk for depression and explored whether differences are affected by vagal activity and pubertal stage.
Methods
We collected clinical assessments, physiological data, and stool samples from 52 adolescents (aged 9-15, including 31 females), consisting of 27 high-risk and 25 low-risk individuals. We used 16S rRNA marker gene sequencing to analyze the diversity, structure, composition, and predicted function of the microbial community. A laboratory stressor task was employed to examine changes in vagally mediated heart rate variability (stress reactivity). Regressions were used to assess the relationship between depression risk, gut microbiota, and cardiovascular stress reactivity indices. Exploratory analyses investigated the effects of sex, age, and pubertal stage (adrenarche and gonarche).
Results
High-risk adolescents exhibited a distinct gut microbiota profile compared to low-risk adolescents, with this effect primarily driven by female participants. This profile was characterized by a higher abundance of Prevotella , which was 2-fold higher in high-risk females, and lower levels of other beneficial genera. High-risk females were also significantly more advanced in adrenarcheal development; the link between depression risk and adrenarcheal development was mediated by gut microbiota in females. Cardiovascular stress reactivity did not differ between groups and was not linked to gut microbiota.
Conclusions
Our results reveal sex-specific links between depression risk, adrenarcheal development, and gut microbiota in adolescence. The increase of Prevotella in high-risk females suggests inflammation-related pathways may connect familial vulnerability to mood disorders. Future long-term studies examining hormones, microbiota, and mood during pubertal changes are essential to determine causality and develop targeted treatments.
