Metabolic profiling of psoriasis vulgaris and palmoplantar pustulosis

Author:

Lee Yujin12,Kim Seong Rae34ORCID,Ban Mu Seong2,Lee Howard2567,Cho Joo‐Youn28,Jo Seong Jin349

Affiliation:

1. Division of Nutritional Sciences Cornell University Ithaca New York USA

2. Department of Clinical Pharmacology and Therapeutics Seoul National University College of Medicine and Hospital Seoul Korea

3. Department of Dermatology Seoul National University College of Medicine Seoul Korea

4. Department of Dermatology Seoul National University Hospital Seoul Korea

5. Department of Molecular Medicine and Biopharmaceutical Sciences, Graduate School of Convergence Science and Technology Seoul National University Seoul Korea

6. Center for Convergence Approaches in Drug Development, Graduate School of Convergence Science and Technology Seoul National University Seoul Korea

7. Advanced Institute of Convergence Technology Suwon Korea

8. Department of Biomedical Sciences Seoul National University College of Medicine Seoul Korea

9. Institute of Human‐Environmental Interface Biology Seoul National University Medical Research Center Seoul Korea

Abstract

AbstractPsoriasis is a chronic inflammatory skin disorder with various subtypes, including psoriasis vulgaris (PV) and palmoplantar pustulosis (PPP). Metabolomics studies have provided insights into psoriasis pathogenesis. However, research on metabolomic alterations in PV and PPP patients is limited. We aimed to explore and compare the metabolic profiles of patients with PV and PPP to those of healthy volunteers (HVs). A single‐centre retrospective cohort was constructed, comprising Korean patients with psoriasis and HVs matched by age and sex. Clinical information including demographics, disease severity, and comorbidities were collected. Plasma samples were subjected to targeted metabolic analysis using an Absolute IDQ®p180 kit, which quantified 188 metabolites, including amino acids and carnitines. Statistical significance was assessed using an independent t‐test and chi‐square test, with p‐values adjusted by the Benjamini–Hochberg procedure. Pathway analyses were employed to gain a comprehensive understanding of the metabolite profile. This study included 93 patients (73 PV and 20 PPP) and an equal number of HVs. PV patients showed increased levels of sarcosine, serotonin, propionylcarnitine, proline, aspartic acid, tyrosine, taurine, spermine and ornithine, but exhibited a decreased level of acetylcarnitine than matched HVs. Notably, sarcosine levels were significantly elevated in PPP patients. Furthermore, the sarcosine/glycine ratio was significantly higher in both PV and PPP patients than in HVs. Pathway analysis showed significant increases in metabolites involved in amino acid metabolism and the urea cycle in PV patients. In conclusion, this study demonstrated distinct metabolic profiles in PV and PPP patients compared to HVs, suggesting sarcosine as a potential biomarker for psoriasis.

Publisher

Wiley

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