Serum metabolomics improves risk stratification for incident heart failure

Rafael R Oexner; Hyunchan Ahn; Konstantinos Theofilatos; Ravi A Shah; Robin Schmitt; Philip Chowienczyk; Anna Zoccarato; Ajay M Shah

doi:10.1002/ejhf.3226

Serum metabolomics improves risk stratification for incident heart failure

Eur J Heart Fail. 2024 Apr;26(4):829-840. doi: 10.1002/ejhf.3226. Epub 2024 Apr 16.

Authors

Rafael R Oexner¹, Hyunchan Ahn¹, Konstantinos Theofilatos¹, Ravi A Shah², Robin Schmitt¹, Philip Chowienczyk¹, Anna Zoccarato¹, Ajay M Shah¹

Affiliations

¹ King's College London British Heart Foundation Centre of Research Excellence, School of Cardiovascular and Metabolic Medicine and Sciences, King's College London, London, UK.
² University College Hospital, University College London Hospitals NHS Foundation Trust, London, UK.

PMID: 38623713
DOI: 10.1002/ejhf.3226

Abstract

Aims: Prediction and early detection of heart failure (HF) is crucial to mitigate its impact on quality of life, survival, and healthcare expenditure. Here, we explored the predictive value of serum metabolomics (168 metabolites detected by proton nuclear magnetic resonance [¹H-NMR] spectroscopy) for incident HF.

Methods and results: Leveraging data of 68 311 individuals and >0.8 million person-years of follow-up from the UK Biobank cohort, we (i) fitted per-metabolite Cox proportional hazards models to assess individual metabolite associations, and (ii) trained and validated elastic net models to predict incident HF using the serum metabolome. We benchmarked discriminative performance against a comprehensive, well-validated clinical risk score (Pooled Cohort Equations to Prevent HF [PCP-HF]). During a median follow-up of ≈12.3 years, several metabolites showed independent association with incident HF (90/168 adjusting for age and sex, 48/168 adjusting for PCP-HF). Performance-optimized risk models effectively retained key predictors representing highly correlated clusters (≈80% feature reduction). Adding metabolomics to PCP-HF improved predictive performance (Harrel's C: 0.768 vs. 0.755, ΔC = 0.013, [95% confidence interval [CI] 0.004-0.022], continuous net reclassification improvement [NRI]: 0.287 [95% CI 0.200-0.367], relative integrated discrimination improvement [IDI]: 17.47% [95% CI 9.463-27.825]). Models including age, sex and metabolomics performed almost as well as PCP-HF (Harrel's C: 0.745 vs. 0.755, ΔC = 0.010 [95% CI -0.004 to 0.027], continuous NRI: 0.097 [95% CI -0.025 to 0.217], relative IDI: 13.445% [95% CI -10.608 to 41.454]). Risk and survival stratification was improved by integrating metabolomics.

Conclusion: Serum metabolomics improves incident HF risk prediction over PCP-HF. Scores based on age, sex and metabolomics exhibit similar predictive power to clinically-based models, potentially offering a cost-effective, standardizable, and scalable single-domain alternative.

Keywords: Biomarker; Heart failure; Prevention; Risk prediction; Screening; Serum metabolomics.

MeSH terms

Aged
Biomarkers / blood
Female
Follow-Up Studies
Heart Failure* / blood
Heart Failure* / epidemiology
Humans
Incidence
Male
Metabolomics* / methods
Middle Aged
Predictive Value of Tests
Risk Assessment / methods
United Kingdom / epidemiology

Substances

Biomarkers

Abstract

MeSH terms

Substances

Grants and funding