Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus

Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus

Abstract Background The pathogenesis of systemic lupus erythematosus (SLE) is poorly understood but has been linked to defective clearance of subcellular particulate material from the circulation. This study investigates the origin, formation, and specificity of circulating microparticles (MPs) in p...

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Main Authors: Ole Østergaard, Christoffer Tandrup Nielsen, Julia T. Tanassi, Line V. Iversen, Søren Jacobsen, Niels H. H. Heegaard
Format: Article
Language:English
Published: BMC 2017-06-01
Series:Clinical Proteomics
Subjects:
Circulating microparticles
Systemic autoimmunity
Systemic lupus erythematosus
Biomarkers
Proteome
Online Access:http://link.springer.com/article/10.1186/s12014-017-9159-8
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spelling doaj-d469de92c6244099859977055122f9fc2020-11-24T23:59:40ZengBMCClinical Proteomics1542-64161559-02752017-06-0114111310.1186/s12014-017-9159-8Distinct proteome pathology of circulating microparticles in systemic lupus erythematosusOle Østergaard0Christoffer Tandrup Nielsen1Julia T. Tanassi2Line V. Iversen3Søren Jacobsen4Niels H. H. Heegaard5Department of Autoimmunology and Biomarkers, Statens Serum InstitutCopenhagen Lupus and Vasculitis Clinic, Centre for Rheumatology and Spine Diseases, Rigshospitalet, Copenhagen University HospitalDepartment of Autoimmunology and Biomarkers, Statens Serum InstitutDepartment of Dermatology, Aarhus University HospitalCopenhagen Lupus and Vasculitis Clinic, Centre for Rheumatology and Spine Diseases, Rigshospitalet, Copenhagen University HospitalDepartment of Autoimmunology and Biomarkers, Statens Serum InstitutAbstract Background The pathogenesis of systemic lupus erythematosus (SLE) is poorly understood but has been linked to defective clearance of subcellular particulate material from the circulation. This study investigates the origin, formation, and specificity of circulating microparticles (MPs) in patients with SLE based on comprehensive MP proteome profiling using patients with systemic sclerosis (SSc) and healthy donors (HC) as controls. Methods We purified MPs from platelet-poor plasma using differential centrifugation of samples from SLE (n = 45), SSc (n = 38), and two sets of HC (n = 35, n = 25). MP proteins were identified and quantitated after trypsin digestion by liquid chromatography-tandem mass spectrometry. The abundance of specific proteins was compared between the groups using univariate statistics and false discovery rate correction for multiple comparisons. Specific proteins and protein ratios were explored for diagnostic and disease activity information using receiver-operating characteristic curves and by analysis of correlations of protein abundance with disease activity scores. Results We identify and quantitate more than 1000 MP proteins and show that a subpopulation of SLE-MPs (which we propose to call luposomes) are highly specific for SLE, i.e. not found in MP preparations from HC or patients with another autoimmune, systemic disease, SSc. In SLE-MPs platelet proteins and mitochondrial proteins are significantly diminished, cytoskeletal proteins deranged, and glycolytic enzymes and apoptotic proteins significantly increased. Conclusions Normal MPs are efficiently removed in SLE, but aberrant MPs, derived from non-lymphoid leukocytes, are less efficiently removed and abundantly produced leading to an altered MP proteome in SLE. The data suggest that an abnormal generation of MPs may partake in the pathology of SLE and that new diagnostic, monitoring, and treatment strategies targeting these processes may be advantageous.http://link.springer.com/article/10.1186/s12014-017-9159-8Circulating microparticlesSystemic autoimmunitySystemic lupus erythematosusBiomarkersProteome
collection DOAJ
language English
format Article
sources DOAJ
author Ole Østergaard
Christoffer Tandrup Nielsen
Julia T. Tanassi
Line V. Iversen
Søren Jacobsen
Niels H. H. Heegaard
spellingShingle Ole Østergaard
Christoffer Tandrup Nielsen
Julia T. Tanassi
Line V. Iversen
Søren Jacobsen
Niels H. H. Heegaard
Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
Clinical Proteomics
Circulating microparticles
Systemic autoimmunity
Systemic lupus erythematosus
Biomarkers
Proteome
author_facet Ole Østergaard
Christoffer Tandrup Nielsen
Julia T. Tanassi
Line V. Iversen
Søren Jacobsen
Niels H. H. Heegaard
author_sort Ole Østergaard
title Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
title_short Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
title_full Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
title_fullStr Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
title_full_unstemmed Distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
title_sort distinct proteome pathology of circulating microparticles in systemic lupus erythematosus
publisher BMC
series Clinical Proteomics
issn 1542-6416
1559-0275
publishDate 2017-06-01
description Abstract Background The pathogenesis of systemic lupus erythematosus (SLE) is poorly understood but has been linked to defective clearance of subcellular particulate material from the circulation. This study investigates the origin, formation, and specificity of circulating microparticles (MPs) in patients with SLE based on comprehensive MP proteome profiling using patients with systemic sclerosis (SSc) and healthy donors (HC) as controls. Methods We purified MPs from platelet-poor plasma using differential centrifugation of samples from SLE (n = 45), SSc (n = 38), and two sets of HC (n = 35, n = 25). MP proteins were identified and quantitated after trypsin digestion by liquid chromatography-tandem mass spectrometry. The abundance of specific proteins was compared between the groups using univariate statistics and false discovery rate correction for multiple comparisons. Specific proteins and protein ratios were explored for diagnostic and disease activity information using receiver-operating characteristic curves and by analysis of correlations of protein abundance with disease activity scores. Results We identify and quantitate more than 1000 MP proteins and show that a subpopulation of SLE-MPs (which we propose to call luposomes) are highly specific for SLE, i.e. not found in MP preparations from HC or patients with another autoimmune, systemic disease, SSc. In SLE-MPs platelet proteins and mitochondrial proteins are significantly diminished, cytoskeletal proteins deranged, and glycolytic enzymes and apoptotic proteins significantly increased. Conclusions Normal MPs are efficiently removed in SLE, but aberrant MPs, derived from non-lymphoid leukocytes, are less efficiently removed and abundantly produced leading to an altered MP proteome in SLE. The data suggest that an abnormal generation of MPs may partake in the pathology of SLE and that new diagnostic, monitoring, and treatment strategies targeting these processes may be advantageous.
topic Circulating microparticles
Systemic autoimmunity
Systemic lupus erythematosus
Biomarkers
Proteome
url http://link.springer.com/article/10.1186/s12014-017-9159-8
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