Serum proteomics of active tuberculosis patients and contacts reveals unique processes activated during Mycobacterium tuberculosis infection

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作者
Jesús Mateos
Olivia Estévez
África González-Fernández
Luis Anibarro
Ángeles Pallarés
Rajko Reljic
Tufária Mussá
Cremildo Gomes-Maueia
Artur Nguilichane
José M. Gallardo
Isabel Medina
Mónica Carrera
机构
[1] Spanish National Research Council (CSIC),Biomedical Research Centre (CINBIO), Galician Singular Center of Research, Galicia Sur Health Research Institute (IIS
[2] University of Vigo,GS), Campus Universitario de Vigo S/N
[3] Tuberculosis Unit,Department of Technologic Platforms
[4] Infectious Diseases,Department of Microbiology, Faculty of Medicine
[5] Internal Medicine Service,undefined
[6] Complexo Hospitalario Universitario de Pontevedra,undefined
[7] Galicia Sur Health Research Institute (IIS-GS,undefined
[8] Mycobacterial Infections Study Group (GEIM) of the Spanish Society of Infectious Diseases and Clinical Microbiology (SEIMC),undefined
[9] St. George’s,undefined
[10] University of London,undefined
[11] Instituto Nacional de Saúde,undefined
[12] Maputo Province,undefined
[13] Eduardo Mondlane University,undefined
[14] Centro de Saúde da Machava II,undefined
[15] Maputo Province,undefined
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摘要
Tuberculosis (TB) is the most lethal infection among infectious diseases. The specific aim of this study was to establish panels of serum protein biomarkers representative of active TB patients and their household contacts who were either infected (LTBI) or uninfected (EMI-TB Discovery Cohort, Pontevedra Region, Spain). A TMT (Tamdem mass tags) 10plex-based quantitative proteomics study was performed in quintuplicate containing a total of 15 individual serum samples per group. Peptides were analyzed in an LC-Orbitrap Elite platform, and raw data were processed using Proteome Discoverer 2.1. A total of 418 proteins were quantified. The specific protein signature of active TB patients was characterized by an accumulation of proteins related to complement activation, inflammation and modulation of immune response and also by a decrease of a small subset of proteins, including apolipoprotein A and serotransferrin, indicating the importance of lipid transport and iron assimilation in the progression of the disease. This signature was verified by the targeted measurement of selected candidates in a second cohort (EMI-TB Verification Cohort, Maputo Region, Mozambique) by ELISA and nephelometry techniques. These findings will aid our understanding of the complex metabolic processes associated with TB progression from LTBI to active disease.
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