What question did this study set out to answer?

The research aims to understand how immune cells and metabolites influence fracture risk through genetic mechanisms.

April 12, 2026Open Access

Unveiling Epigenetic Molecular Mechanisms in Bone Fracture Risk: Insights From 731 Immune Cells, 1400 Metabolites, and Critical Genetic Pathways

Key Points

The research aims to understand how immune cells and metabolites influence fracture risk through genetic mechanisms.
Analysis of immune cell data and metabolite profiling in relation to fracture risk.
Identification of critical genetic pathways and hub genes associated with fractures.
Assessment of fracture-associated single nucleotide polymorphisms (SNPs) and their epigenetic regulation.
Immune cells and metabolites show genetically predicted effects on fracture risk.
Critical pathways and hub genes linked to fractures were identified.
Potential mediators include metabolites through epigenetic regulation at specific methylation sites.

Abstract

The findings suggest that immune cells and metabolites may have genetically predicted effects on fracture risk, with metabolites potentially serving as key mediators. Critical pathways, hub genes, and fracture-associated SNPs were identified, along with potential epigenetic regulation via methylation sites. These preliminary insights offer novel directions for future research into the underlying mechanisms of fracture risk and intervention.

Unveiling Epigenetic Molecular Mechanisms in Bone Fracture Risk: Insights From 731 Immune Cells, 1400 Metabolites, and Critical Genetic Pathways

Key Points

Abstract

Cite This Study