Systemic lupus erythematosus patients have unique changes in serum metabolic profiles across age associated with cardiometabolic risk

Elizabeth C Jury; Junjie Peng; Alexandra Van Vijfeijken; Lucia Martin Gutierrez; Laurel Woodridge; Chris Wincup; Ines Pineda-Torra; Coziana Ciurtin; George A Robinson

doi:10.1093/rheumatology/kead646

Systemic lupus erythematosus patients have unique changes in serum metabolic profiles across age associated with cardiometabolic risk

Rheumatology (Oxford). 2023 Dec 4:kead646. doi: 10.1093/rheumatology/kead646. Online ahead of print.

Authors

Elizabeth C Jury¹, Junjie Peng², Alexandra Van Vijfeijken¹, Lucia Martin Gutierrez^{1

2}, Laurel Woodridge^{3

4}, Chris Wincup¹, Ines Pineda-Torra³, Coziana Ciurtin^{1

2}, George A Robinson^{1

2}

Affiliations

¹ Centre for Rheumatology Research, Division of Medicine, University College London, London, UK.
² Centre for Adolescent Rheumatology Versus Arthritis, Division of Medicine, University College London, London, UK.
³ Centre for Experimental & Translational Medicine, Division of Medicine, University College London, London, UK.
⁴ Institute of Structural and Molecular Biology, University College London, London, UK.

PMID: 38048621
DOI: 10.1093/rheumatology/kead646

Abstract

Objectives: Cardiovascular disease through accelerated atherosclerosis is a leading cause of mortality for patients with systemic lupus erythematosus (SLE), likely due to increased chronic inflammation and cardiometabolic defects over age. We investigated age-associated changes in metabolomic profiles of SLE patients and healthy controls (HCs).

Methods: Serum NMR metabolomic profiles from female SLE patients (n = 164, age = 14-76) and HCs (n = 123, age = 13-72) were assessed across age by linear regression and by age group between patients/HCs (Group-1, age ≤ 25, n = 62/46; Group-2, age = 26-49, n = 50/46; Group-3, age ≥ 50, n = 52/31) using multiple t-tests. The impact of inflammation, disease activity and treatments were assessed, and UK Biobank disease-wide association analysis of metabolites was performed.

Results: Age-specific metabolomic profiles were identified in SLE patients vs HCs, including reduced amino acids (Group-1), increased very-low-density lipoproteins (Group-2), and increased low-density lipoproteins (Group-3). Twenty-five metabolites were significantly altered in all SLE age groups, dominated by decreased atheroprotective high-density lipoprotein (HDL) subsets, HDL-bound apolipoprotein(Apo)A1 and increased glycoprotein acetyls (GlycA). Furthermore, ApoA1 and GlycA were differentially associated with disease activity and serological measures, as well as atherosclerosis incidence and myocardial infarction mortality risk through disease-wide association. Separately, glycolysis pathway metabolites (acetone/citrate/creatinine/glycerol/lactate/pyruvate) uniquely increased with age in SLE, significantly influenced by prednisolone (increased pyruvate/lactate) and hydroxychloroquine (decreased citrate/creatinine) treatment and associated with type-1 and type-2 diabetes by disease-wide association.

Conclusions: Increasing HDL (ApoA1) levels through therapeutic/nutritional intervention, whilst maintaining low disease activity, in SLE patients from a young age could improve cardiometabolic disease outcomes. Biomarkers from the glycolytic pathway could indicate adverse metabolic effects of current therapies.

Keywords: SLE; age; atherosclerosis; cardiometabolic; cardiovascular disease; comorbidities; lipids; metabolism; metabolomics.

Grants and funding

22856/VAC_/Versus Arthritis/United Kingdom