Proteomic profiling of human plasma extracellular vesicles identifies PF4 and C1R as novel biomarker in sarcopenia

Author:

Aparicio Paula1234ORCID,Navarrete‐Villanueva David456,Gómez‐Cabello Alba457,López‐Royo Tresa1234,Santamaría Enrique8,Fernández‐Irigoyen Joaquín8,Ausín Karina8,Arruebo Manuel4910,Sebastian Victor491011,Vicente‐Rodríguez Germán451213,Osta Rosario1234,Manzano Raquel1234ORCID

Affiliation:

1. LAGENBIO Laboratory, Faculty of Veterinary University of Zaragoza Zaragoza Spain

2. Centre for Biomedical Research in Neurodegenerative Diseases (CIBERNED) Instituto de Salud Carlos III Madrid Spain

3. AgroFood Institute of Aragon (IA2) Zaragoza Spain

4. Aragon Health Research Institute (IIS Aragon) Zaragoza Spain

5. EXER‐GENUD (Growth, Exercise, Nutrition and Development) Research Group University of Zaragoza Zaragoza Spain

6. Faculty of Health Science University of Zaragoza Zaragoza Spain

7. Defense University Center Zaragoza Spain

8. Proteomics Platform, Clinical Neuroproteomics Unit, Navarrabiomed Hospital Universitario de Navarra (HUN), Instituto de Investigación Sanitaria de Navarra (IdiSNA) Pamplona Spain

9. Instituto de Nanociencia y Materiales de Aragón (INMA) CSIC‐Universidad de Zaragoza Zaragoza Spain

10. Department of Chemical and Environmental Engineering University of Zaragoza, Campus Río Ebro‐Edificio I+D Zaragoza Spain

11. Networking Research Center on Bioengineering, Biomaterials and Nanomedicine CIBER‐BBN Madrid Spain

12. Centro de Investigación Biomédica en Red de Fisiopatología de la Obesidad y Nutrición (CIBERObn) Madrid Spain

13. Faculty of Health and Sport Science (FCSD), Department of Physiatry and Nursing University of Zaragoza Zaragoza Spain

Abstract

AbstractBackgroundSarcopenia, the gradual and generalized loss of muscle mass and function with ageing, is one of the major health problems in older adults, given its high prevalence and substantial socioeconomic implications. Despite the extensive efforts to reach consensus on definition and diagnostic tests and cut‐offs for sarcopenia, there is an urgent and unmet need for non‐invasive, specific and sensitive biomarkers for the disease. Extracellular vesicles (EVs) are present in different biofluids including plasma, whose cargo reflects cellular physiology. This work analysed EV proteome in sarcopenia and robust patients in the search for differentially contained proteins that can be used to diagnose the disease.MethodsPlasma small EVs (sEVs) from a total of 29 robust controls (aged 73.4 ± 5.6 years; 11 men and 18 women) and 49 sarcopenic patients (aged 82.3 ± 5.4 years; 15 men and 34 women) aged 65 years and older were isolated and their cargo was analysed by proteomics. Proteins whose concentration in sEVs was different between sarcopenic and robust patients were further validated using ELISA. The concentration of these candidates was correlated to the EWGSOP2 sarcopenia tests for low muscle strength and low physical performance, and receiver operating characteristic (ROC) curve analyses were carried out to evaluate their diagnostic power, sensitivity and specificity.ResultsProteomic analysis identified 157 sEVs proteins in both sarcopenic and robust samples. Among them, 48 proteins had never been reported in the ExoCarta nor Vesiclepedia databases. Statistical analysis revealed eight proteins whose concentration was significantly different between groups: PF4 (log2 FC = 4.806), OIT3 (log2 FC = −1.161), MMRN1 (log2 FC = −1.982), MASP1 (log2 FC = −0.627), C1R (log2 FC = 1.830), SVEP1 (log2 FC = 1.295), VCAN (FC = 0.937) and SPTB (log2 FC = 1.243). Among them, platelet factor 4 (PF4) showed the lowest concentration while Complement C1r subcomponent (C1R) increased the most in sarcopenic patients, being these results confirmed by ELISA (P = 1.07E‐09 and P = 0.001287, respectively). The concentrations of candidate proteins significantly correlated with EWGSOP2 tests currently used. ROC curve analysis showed an area under the curve of 0.8921 and 0.7476 for PF4 and C1R, respectively. Choosing the optimal for PF4, 80% sensitivity and 85.71% specificity was reached while the optimal cut‐off value of C1R would allow sarcopenia diagnosis with 75% sensitivity and 66.67% specificity.ConclusionsOur results support the determination of EV PF4 and C1R as plasma diagnostic biomarkers in sarcopenia and open the door to investigate the role of the content of these vesicles in the pathogeny of the disease.

Funder

Universidad de Zaragoza

Ministerio de Asuntos Económicos y Transformación Digital, Gobierno de España

Publisher

Wiley

Reference40 articles.

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