Proteomic Associations and Signatures of Frailty Among Older Men
Jodi Lapidus, Alicia Feryn, Jack Wiendrick, Adam Burns, Eric Orwoll, Kristine Ensrud

TL;DR
This study identifies proteins linked to frailty in older men, offering insights into biological networks involved in aging-related frailty.
Contribution
The study introduces multi-protein signatures and identifies novel proteins associated with frailty and its components in older men.
Findings
Seventy-six proteins showed strong associations with frailty in older men.
Frailty-related proteins include those involved in inflammation, DNA repair, and tissue repair.
Proteins like C/EBPβ, ARIDA1, and APP were specifically linked to frailty components.
Abstract
Aging leads to biological changes that influence frailty onset and prevalence, and these changes are likely reflected in circulating proteins. In this study, we analyzed serum proteomics (SomaLogic 7K panel) from 500 older men (average age 84 ± 3.4 years) in the MrOS study at the fourth visit in 2015. A phenotypic frailty index was computed, including several components: shrinkage (recent weight loss, low BMI), weakness (grip strength <32 kg), low energy, slowness (gait speed <0.8 m/s, use of a walking aid), and low physical activity (no walking for exercise). Participants were classified as robust (22%), intermediate (58%), or frail (20%). Our objective was to identify proteins and co-expression protein modules linked to frailty and create multi-protein signatures of frailty. Seventy-six proteins showed consistent associations with frailty (e.g., odds ratio > |1.5| or standardized…
Genes, proteins, chemicals, diseases, species, mutations and cell lines named across the full text — each resolved to its canonical identifier and authoritative record.
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Taxonomy
TopicsGDF15 and Related Biomarkers · Clusterin in disease pathology · Frailty in Older Adults
