What question did this study set out to answer?

This research aims to explore how lifelong low social status influences inflammatory responses in female macaques.

January 18, 2026Open Access

Effects of Lifelong Low Social Status on Inflammatory Markers in Adult Female Macaques—Long-Term Inflammatory Effects of Low Social Status on Adult Macaques

Puntos clave

This research aims to explore how lifelong low social status influences inflammatory responses in female macaques.
Examined inflammatory markers in socially housed female rhesus macaques over different life stages: infancy, juvenile, and adulthood.
Collected baseline blood samples and assessed pro- and anti-inflammatory markers before and after lipopolysaccharide (LPS) immune challenge.
Measured cortisol levels to understand its relationship with inflammation and HPA axis activity.
SUB macaques exhibited a specific immune response to LPS, revealing higher IL-1β, IL-2, and IL-10 levels than DOM macaques.
IL-8 response was lower in SUB compared to DOM animals in adulthood.
Cortisol levels were significantly higher during infancy than adulthood, with no major impact from social rank.

Resumen

Low social status leads to chronic social stress that predicts risk for physical and mental illness, especially when it starts early in life. To examine the longitudinal effects of low social status on the immune system, this study assessed the effects of low social status on developmental secretory patterns of pro- and anti-inflammatory markers under baseline conditions, as well as in response to an immune challenge (lipopolysaccharide (LPS)-induced activation of pro- and anti-inflammatory cytokines) in a translational rhesus monkey model of lifelong social subordination stress. Baseline blood samples were collected in 27 socially housed female rhesus monkeys (13 dominants, DOM, and 14 subordinates, SUB) during infancy (6 months), the juvenile pre-pubertal period (16 months), and adulthood (9–10 years) to examine the longitudinal effects of social status on inflammatory markers in unstimulated versus LPS-stimulated conditions mimicking exposure to bacterial infection. Basal levels of the stress hormone cortisol in blood were measured to examine associations between inflammation and activity of the hypothalamic–pituitary–adrenal (HPA) axis throughout the life span. Basal peripheral levels of inflammatory markers (e.g., IL-6) increased across development in both SUB and DOM animals with no significant differences. Basal cortisol levels were significantly higher in infancy as compared to adulthood, but no significant effects of social rank were detected. However, in adulthood, SUB animals showed a cytokine-specific immune response to ex vivo LPS stimulation with significantly higher secretions of IL-1β, IL-2, and IL-10 compared to DOM animals, whereas IL-8 response to LPS was lower in SUB animals than in DOMs. This cytokine-specific response to an immune challenge that mimics bacterial infection could reflect dysregulated immune cells that may have short-term adaptation, but at the cost of longer-term risks for low-grade chronic inflammation and accelerated immune aging for socially subordinate female macaques.

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Cite This Study

Sánchez et al. (Fri,) studied this question.

synapsesocial.com/papers/696c77afeb60fb80d1395e25 https://doi.org/https://doi.org/10.3390/biom16010159

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