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Abstract Number: 0901

Data-Driven Metabolomics Identifies Diagnostic Signatures and Patient Subgroups in Systemic Autoimmune Disorders

Chary López pedrera1, Antonio Perez-Campoamor2, Gema Dolores García-Delgado3, Beatriz Vellón-García4, Adrián Llamas Urbano5, Laura Romero Zurita6, Pedro Ortiz Buitrago7, Christian Merlo8, Maria del carmen abalos-aguilera8, Nuria Barbarroja9, Verónica Bolón-Canedo10, MARIA ANGELES AGUIRRE ZAMORANO11, Rafaela Ortega-Castro12, Jerusalén Calvo13, Lourdes Ladehesa14, Marta Alarcon-Riquelme15, Alejandro Escudero-contreras8 and Carlos Pérez Sánchez16, 1Rheumatology service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ Reina Sofia University Hospital/ University of Cordoba, Spain, Cordoba, Spain, 2STARTQUAKE S.L., Gijón, Spain/Research Center on Information and Communication Technologies (CITIC), University of A Coruña, A Coruña, Spain, Gijón, Spain, 3Rheumatology Service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/University of Cordoba/ Reina Sofia University Hospital, Córdoba, Spain/Department of Cell Biology, Physiology and Immunology, Maimonides Institute of Biomedical Research of Cordoba (IMIBIC), Reina Sofia University Hospital, University of Cordoba, Cordoba, Spain., Cordoba, Spain, 4Rheumatology Service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/University of Cordoba/ Reina Sofia University Hospital, Córdoba, Spain/Department of Cell Biology, Physiology and Immunology, Maimonides Institute of Biomedical Research of Cordoba (IMIBIC), Reina Sofia University Hospital, University of Córdoba, Córdoba, Spain, Cordoba, Spain, 5Cobiomic Bioscience SL. EBT University of Cordoba/IMIBIC, Cordoba, Spain., Cordoba, Spain, 6Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ University of Cordoba/ Reina Sofia University Hospital, Rheumatology service/Department of Medical and Surgical Sciences, Cordoba, Spain, Córdoba, Spain, 7Maimonides Institute of Biomedical Research of Córdoba (IMIBIC), Cordoba, Andalucia, Spain, 8Rheumatology Service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/University of Cordoba/ Reina Sofia University Hospital, Córdoba, Spain, Cordoba, Spain, 9Rheumatology service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ Reina Sofia University Hospital/ University of Cordoba, Spain/CobiomicBioscience S.l, Cordoba, Spain, Cordoba, Spain, 10Research Center on Information and Communication Technologies (CITIC), University of A Coruña, A Coruña, Spain, A coruña, Spain, 11Rheumatology service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ Reina Sofia University Hospital/ University of Cordoba, Spain, Córdoba, Spain, 12Rheumatology service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ Reina Sofia University Hospital/ University of Cordoba, Spain, Cordoba, Andalucia, Spain, 13IMIBIC / Reina Sofia Hospital / University of Cordoba, Córdoba, Spain, 14IMIBIC-Reina Sofia Hospital-University of Cordoba, Cordoba, Spain, Cordoba, Spain, 15Fundación Progreso y Salud, Andalusian Government, Granada, Spain, 16Rheumatology service/Maimonides Institute for Research in Biomedicine of Cordoba (IMIBIC)/ Reina Sofia University Hospital/ University of Cordoba, Spain/ CobiomicBioscience S.l, Cordoba, Spain, Cordoba, Spain

Meeting: ACR Convergence 2025

Keywords: autoimmune diseases, Bioinformatics, Biomarkers, metabolomics

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Session Information

Date: Monday, October 27, 2025

Title: (0897–0915) B Cell Biology & Targets in Autoimmune & Inflammatory Disease Poster II

Session Type: Poster Session B

Session Time: 10:30AM-12:30PM

Background/Purpose: This study aims to characterize the metabolomic fingerprint of several systemic autoimmune diseases (SADs) and apply machine learning (ML) techniques to identify disease-specific biomarkers and improve patient diagnosis and stratification.

Methods: A total of 716 individuals from the PRECISESADS study, were analyzed, including 272 with rheumatoid arthritis (RA), 183 with systemic lupus erythematosus (SLE), 148 with primary antiphospholipid syndrome (PAPS), 70 with systemic sclerosis (SSc), and 43 healthy donors (HDs). Serum metabolomic profiles were assessed using nuclear magnetic resonance (Nightingale), alongside extensive clinical and analytical data. A combination of ML approaches, including unsupervised patient stratification, and a supervised Logistic Regression using 5-Fold Cross Validation was used to identify potential diagnostic signatures. Correlation analyses explored associations between metabolic alterations and clinical features.

Results: Several metabolites (metabs) were differentially expressed in each disease compared to HDs, with the most alterations in SSc (99 metabs) and APS (68 metabs), followed by SLE (30 metabs) and RA (17 metabs). Notably, some cardiovascular-related metabolites (e.g., histidine, albumin, L-LDL-C, L-LDL-CE) were simultaneously altered across all diseases, while each also exhibited unique metabolic change. ML generated disease-specific diagnostic signatures with AUCs above 0.8 in all cases.Unsupervised clustering analysis of the entire cohort identified three patient clusters (C1, C2, C3), with each disease represented across all clusters in varying proportions. C1 showed significant differences compared to C3 in both clinical features and metabolomic profiles, while C2 represented an intermediate group. Patients in C1 had increased cardiovascular risk markers compared with C3, while C2 represented an intermediate group.In APS, C1 was linked to higher thrombotic risk (aGAPSS), arterial events, and metabolic comorbidities, while C2 showed more venous thrombosis and pregnancy complications. In SLE, C1 had more cardiovascular risk factors, lupus nephritis, and anti-dsDNA positivity than C3. In RA, C1 showed higher rates of obesity, diabetes, and atherosclerosis, whereas C3 had greater disease activity and autoantibody positivity. In SSc, C1 was associated with dyslipidemia, lung fibrosis, and anti-U1-RNP, while C3 had more skin involvement and anti-centromere positivity.

Conclusion: Distinct metabolomic profiles were identified with shared and disease-specific alterations across systemic autoimmune diseases. ML revealed accurate diagnostic signatures and uncovered patient subgroups with unique clinical and metabolomic features, highlighting shared pathogenic mechanisms and disease-specific features and supporting the potential for personalized therapies targeting metabolic pathways.Supported by CPS: RYC2021-033828-I; PID2022-141500OA-I00; DIN2022-012766 Minister of Science, Innovation and Universities co-financed by the European Union; and CLP: (PI24/00959, CD21/00187 and RICOR-24/0007/0019), co-financed by European Union. EU/EFPIA-IMI-PRECISESADS (n° 115565)


Disclosures: C. López pedrera: None; A. Perez-Campoamor: None; G. García-Delgado: None; B. Vellón-García: None; A. Llamas Urbano: None; L. Romero Zurita: None; P. Ortiz Buitrago: None; C. Merlo: None; M. abalos-aguilera: None; N. Barbarroja: None; V. Bolón-Canedo: None; M. AGUIRRE ZAMORANO: None; R. Ortega-Castro: None; J. Calvo: None; L. Ladehesa: None; M. Alarcon-Riquelme: None; A. Escudero-contreras: None; C. Pérez Sánchez: None.

To cite this abstract in AMA style:

López pedrera C, Perez-Campoamor A, García-Delgado G, Vellón-García B, Llamas Urbano A, Romero Zurita L, Ortiz Buitrago P, Merlo C, abalos-aguilera M, Barbarroja N, Bolón-Canedo V, AGUIRRE ZAMORANO M, Ortega-Castro R, Calvo J, Ladehesa L, Alarcon-Riquelme M, Escudero-contreras A, Pérez Sánchez C. Data-Driven Metabolomics Identifies Diagnostic Signatures and Patient Subgroups in Systemic Autoimmune Disorders [abstract]. Arthritis Rheumatol. 2025; 77 (suppl 9). https://acrabstracts.org/abstract/data-driven-metabolomics-identifies-diagnostic-signatures-and-patient-subgroups-in-systemic-autoimmune-disorders/. Accessed .
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