Metabolomic Biomarker Candidates for Skeletal Muscle Loss in the Collagen-Induced Arthritis (CIA) Model

Paulo V. G. Alabarse; Jordana M. S. Silva; Rafaela C. E. Santo; Marianne S. Oliveira; Andrelise S. Almeida; Mayara S. de Oliveira; Mônica L. Immig; Eduarda C. Freitas; Vivian O. N. Teixeira; Camilla L. Bathurst; Claiton V. Brenol; Lidiane I. Filippin; Stephen P. Young; Priscila S. Lora; Ricardo M. Xavier

doi:10.3390/jpm11090837

Journal of Personalized Medicine (Aug 2021)

Metabolomic Biomarker Candidates for Skeletal Muscle Loss in the Collagen-Induced Arthritis (CIA) Model

Paulo V. G. Alabarse,
Jordana M. S. Silva,
Rafaela C. E. Santo,
Marianne S. Oliveira,
Andrelise S. Almeida,
Mayara S. de Oliveira,
Mônica L. Immig,
Eduarda C. Freitas,
Vivian O. N. Teixeira,
Camilla L. Bathurst,
Claiton V. Brenol,
Lidiane I. Filippin,
Stephen P. Young,
Priscila S. Lora,
Ricardo M. Xavier

Affiliations

Paulo V. G. Alabarse: VA San Diego Healthcare System, Veteran Medical Research Foundation, San Diego, CA 92161, USA
Jordana M. S. Silva: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Rafaela C. E. Santo: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Marianne S. Oliveira: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Andrelise S. Almeida: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Mayara S. de Oliveira: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Mônica L. Immig: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Eduarda C. Freitas: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Vivian O. N. Teixeira: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Camilla L. Bathurst: Queen Elizabeth Hospital and National Institute for Health Research, Birmingham Biomedical Research Centre, University of Birmingham, Birmingham B15 2TT, UK
Claiton V. Brenol: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil
Lidiane I. Filippin: Universidade La Salle, Canoas 92010-000, Brazil
Stephen P. Young: Queen Elizabeth Hospital and National Institute for Health Research, Birmingham Biomedical Research Centre, University of Birmingham, Birmingham B15 2TT, UK
Priscila S. Lora: Universidade do Vale do Rio dos Sinos, São Leopoldo 93022-750, Brazil
Ricardo M. Xavier: Hospital de Clínicas de Porto Alegre, Serviço de Reumatologia, Laboratório de Doenças Autoimunes, Porto Alegre 90035-903, Brazil

DOI: https://doi.org/10.3390/jpm11090837
Journal volume & issue: Vol. 11, no. 9
p. 837

Abstract

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There is no consensus for diagnosis or treatment of RA muscle loss. We aimed to investigate metabolites in arthritic mice urine as biomarkers of muscle loss. DBA1/J mice comprised collagen-induced arthritis (CIA) and control (CO) groups. Urine samples were collected at 0, 18, 35, 45, 55, and 65 days of disease and subjected to nuclear magnetic resonance spectroscopy. Metabolites were identified using Chenomx and Birmingham Metabolite libraries. The statistical model used principal component analysis, partial least-squares discriminant analysis, and partial least-squares regression analysis. Linear regression and Fisher’s exact test via the MetaboAnalyst website were performed (VIP-score). Nearly 100 identified metabolites had CIA vs. CO and disease time-dependent differences (p 2) and succinyl acetone (VIPs 1.0 × 10) showed high importance in CIA vs. CO models at day 65; CIA pair analysis showed histidine (VIPs 1.2 × 102) days 55 vs. 65, histamine (VIPs 1.1 × 102) days 55 vs. 65, and L-methionine (VIPs 1.1 × 102) days 0 vs. 18. Carnosine was fatigue- (0.039) related, creatine was food intake- (−0.177) and body weight- (−0.039) related, and both metabolites were clinical score- (0.093; 0.050) and paw edema- (0.125; 0.026) related. Therefore, muscle metabolic alterations were detected in arthritic mice urine, enabling further validation in RA patient’s urine, targeting prognosis, diagnosis, and monitoring of RA-mediated muscle loss.

Published in Journal of Personalized Medicine

ISSN: 2075-4426 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine
Website: http://www.mdpi.com/journal/jpm

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