# Metabolic resilience governs sex-specific pain recovery during hormonal aging: a multi-omics study of neuropathy in mice

**Authors:** Sara Marinelli, Claudia Rossi, Luisa Pieroni, Giacomo Giacovazzo, Valentina Vacca, Federica De Angelis, Ilaria Cicalini, Valentina Mastrorilli, Chiara Parisi, Zuleyha Nihan Yurtsever, Domenico Ciavardelli, Roberto Coccurello

PMC · DOI: 10.3389/fpain.2025.1655712 · 2025-10-13

## TL;DR

Aging and sex influence metabolic changes that affect pain recovery differently in males and females, with females showing better recovery during hormonal aging.

## Contribution

The study reveals sex-specific metabolic adaptations during aging that govern pain recovery after nerve injury.

## Key findings

- Aging females showed increased fatty acid oxidation and metabolic flexibility, aiding pain recovery.
- Males exhibited metabolic inflexibility with glycolytic reliance and reduced adiponectin and PPARγ.
- Females recovered more fully from nerve injury compared to males during hormonal aging.

## Abstract

Biological aging and sex interact to shape systemic metabolism, yet their role in chronic pain resolution remains unexplored. We hypothesized that metabolic resilience—the ability to flexibly switch fuel sources and maintain energy homeostasis—rules successful recovery from nerve injury in a sex-dependent manner during aging.

In 12-month-old male and female mice, corresponding to the perimenopausal phase in females and the onset of hormonal decline in both sexes, we induced sciatic nerve chronic constriction injury and performed multi-omics profiling during Wallerian degeneration, a phase known to trigger long-term neurobiological remodeling.

Aging females exhibited early activation of fatty acid oxidation, increased resting energy expenditure, upregulation of mitochondrial redox enzymes and circulating progesterone and corticosterone. Proteomic and metabolomic analysis revealed pentose phosphate pathway enrichment and gluconeogenesis, supporting redox balance and metabolic flexibility. Conversely, males displayed persistent glycolytic reliance, long-chain acylcarnitine accumulation, suppression of adiponectin and PPARγ, indicating metabolic inflexibility. Longitudinal behavioral analysis revealed that aging females recovered earlier and more fully than aging males, reversing the pattern previously shown in our adult mouse study, where females developed persistent pain and males recovered rapidly.

These patterns highlight a non-linear, sex-specific interaction between biological aging and injury response, where hormonal decline reprograms the metabolic trajectory and reshapes pain outcomes. Metabolic resilience governs sex-specific recovery following nerve injury by directing early systemic adaptations that precede and predict long-term pain trajectories. These results define mechanistically anchored, sex- and age-specific biomarkers, and propose preclinical targets for timely, personalized interventions in age-associated neuropathic pain.

## Linked entities

- **Proteins:** PPARG (peroxisome proliferator activated receptor gamma)
- **Species:** Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** Pparg (peroxisome proliferator activated receptor gamma) [NCBI Gene 19016] {aka Nr1c3, PPAR-gamma, PPAR-gamma2, PPARgamma, PPARgamma2}, Adipoq (adiponectin, C1Q and collagen domain containing) [NCBI Gene 11450] {aka 30kDa, APN, Acdc, Acrp30, Ad, Adid}
- **Diseases:** pain (MESH:D010146), sciatic nerve chronic constriction injury (MESH:D020426), nerve injury (MESH:D000080902), chronic pain (MESH:D059350), Wallerian degeneration (MESH:D014855), neuropathy (MESH:D009422), neuropathic pain (MESH:D009437)
- **Chemicals:** corticosterone (MESH:D003345), progesterone (MESH:D011374), fatty acid (MESH:D005227), pentose phosphate (MESH:D010428), -chain acylcarnitine (-)
- **Species:** Mus musculus (house mouse, species) [taxon 10090]

## Figures

10 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12554762/full.md

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Source: https://tomesphere.com/paper/PMC12554762