Fibrinogen-Associated Plasma Metabolites and Implications for Coagulation, Inflammation, and Vascular Diseases

  1. Jayna C. Nicholas
  2. Taryn Alkis
  3. Joshua C. Bis
  4. Eric Boerwinkle
  5. Jennifer A. Brody
  6. Clary B. Clish
  7. Paul S. de Vries
  8. Yan Gao
  9. Robert E. Gerzsten
  10. Xiuqing Guo
  11. Andrew D. Johnson
  12. Martin G. Larson
  13. Rozenn N. Lemaitre
  14. Bruce M. Psaty
  15. Vasan Ramachandran
  16. Alexander P. Reiner
  17. Stephen S. Rich
  18. Benjamin Rodriguez
  19. Jian Rong
  20. Jerome I. Rotter
  21. Jeanette Simino
  22. Nicholas L. Smith
  23. James Wilson
  24. Jie Yao
  25. Alanna C. Morrison
  26. Bing Yu
  27. Laura M. Raffield
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Abstract

Background

Fibrinogen is a critical coagulation factor that plays an essential role in thrombosis and is elevated in individuals with chronic inflammation. Here, we used fibrinogen as a representative quantitative measure of pro-coagulant risk and evaluated metabolites associated with fibrinogen levels through non-targeted plasma metabolomic profiling (Broad and Metabolon platforms).

Methods

Our analysis included 10,533 individuals across six U.S. based cohorts representing diverse population groups. The cross-sectional relationship between each of 789 tested metabolites and plasma fibrinogen concentration was assessed with adjustment for relevant covariates such as age, sex, body mass index, and circulating lipoprotein levels.

Results

Meta-analysis of per-cohort results revealed 270 metabolites significantly associated with fibrinogen level (FDR adjusted p-value < 0.05). Lipid species such as glycerophospholipids, sphingolipids, and fatty acyls were prevalent among significantly associated metabolites; some of these may capture effects of inflammation, as supported by sensitivity analyses adjusted for C-reactive protein. Significant associations between fibrinogen levels and serotonin, thyroxine, and sex-hormone derivatives may capture endogenous influences on fibrinogen levels. Exogenous compounds and microbial co-metabolites significantly associated with fibrinogen also implicate lifestyle and microbiome risk-factors. Only a portion of fibrinogen-associated metabolites (30%) have been associated with a cardiovascular disease outcome in a prior study, suggesting the associations discovered here may provide insights on vascular biology which case-control studies may not yet be powered to detect.

Conclusions

These findings contribute to a growing list of metabolite biomarkers that may influence coagulation and inflammation pathways and may thereby contribute to vascular risk.

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  1. Version published to 10.1101/2025.08.06.25333064 on medRxiv