Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers

INTRODUCTION: Early systemic sclerosis (SSc) is characterized by Raynaud's phenomenon together with scleroderma marker autoantibodies and/or a scleroderma pattern at capillaroscopy and no other distinctive feature of SSc. Patients presenting with marker autoantibodies plus a capillaroscopic scl...

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Autores principales: Valentini, Gabriele, Marcoccia, Antonella, Cuomo, Giovanna, Vettori, Serena, Iudici, Michele, Bondanini, Francesco, Santoriello, Carlo, Ciani, Aldo, Cozzolino, Domenico, De Matteis, Giovanni Maria, Cappabianca, Salvatore, Vitelli, Filiberto, Spanò, Alberto
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4060381/
https://www.ncbi.nlm.nih.gov/pubmed/23718566
http://dx.doi.org/10.1186/ar4236
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author Valentini, Gabriele
Marcoccia, Antonella
Cuomo, Giovanna
Vettori, Serena
Iudici, Michele
Bondanini, Francesco
Santoriello, Carlo
Ciani, Aldo
Cozzolino, Domenico
De Matteis, Giovanni Maria
Cappabianca, Salvatore
Vitelli, Filiberto
Spanò, Alberto
author_facet Valentini, Gabriele
Marcoccia, Antonella
Cuomo, Giovanna
Vettori, Serena
Iudici, Michele
Bondanini, Francesco
Santoriello, Carlo
Ciani, Aldo
Cozzolino, Domenico
De Matteis, Giovanni Maria
Cappabianca, Salvatore
Vitelli, Filiberto
Spanò, Alberto
author_sort Valentini, Gabriele
collection PubMed
description INTRODUCTION: Early systemic sclerosis (SSc) is characterized by Raynaud's phenomenon together with scleroderma marker autoantibodies and/or a scleroderma pattern at capillaroscopy and no other distinctive feature of SSc. Patients presenting with marker autoantibodies plus a capillaroscopic scleroderma pattern seem to evolve into definite SSc more frequently than patients with either feature. Whether early SSc patients with only marker autoantibodies or capillaroscopic positivity differ in any aspect at presentation is unclear. METHODS: Seventy-one consecutive early SSc patients were investigated for preclinical cardiopulmonary alterations. Out of these, 44 patients and 25 controls affected by osteoarthritis or primary fibromyalgia syndrome were also investigated for serum markers of fibroblast (carboxyterminal propeptide of collagen I), endothelial (soluble E-selectin) and T-cell (soluble IL-2 receptor alpha) activation. RESULTS: Thirty-two of the 71 patients (45.1%) had both a marker autoantibody and a capillaroscopic scleroderma pattern (subset 1), 16 patients (22.5%) had only a marker autoantibody (subset 2), and 23 patients (32.4%) had only a capillaroscopic scleroderma pattern (subset 3). Patients with marker autoantibodies (n = 48, 67.6%) had a higher prevalence of impaired diffusing lung capacity for carbon monoxide (P = 0.0217) and increased serum levels of carboxyterminal propeptide of collagen I (P = 0.0037), regardless of capillaroscopic alterations. Patients with a capillaroscopic scleroderma pattern (n = 55, 77.5%) had a higher prevalence of puffy fingers (P = 0.0001) and increased serum levels of soluble E-selectin (P = 0.0003) regardless of marker autoantibodies. CONCLUSION: These results suggest that the autoantibody and microvascular patterns in early SSc may each be related to different clinical-preclinical features and circulating activation markers at presentation. Longitudinal studies are warranted to investigate whether these subsets undergo a different disease course over time.
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spelling pubmed-40603812014-06-17 Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers Valentini, Gabriele Marcoccia, Antonella Cuomo, Giovanna Vettori, Serena Iudici, Michele Bondanini, Francesco Santoriello, Carlo Ciani, Aldo Cozzolino, Domenico De Matteis, Giovanni Maria Cappabianca, Salvatore Vitelli, Filiberto Spanò, Alberto Arthritis Res Ther Research Article INTRODUCTION: Early systemic sclerosis (SSc) is characterized by Raynaud's phenomenon together with scleroderma marker autoantibodies and/or a scleroderma pattern at capillaroscopy and no other distinctive feature of SSc. Patients presenting with marker autoantibodies plus a capillaroscopic scleroderma pattern seem to evolve into definite SSc more frequently than patients with either feature. Whether early SSc patients with only marker autoantibodies or capillaroscopic positivity differ in any aspect at presentation is unclear. METHODS: Seventy-one consecutive early SSc patients were investigated for preclinical cardiopulmonary alterations. Out of these, 44 patients and 25 controls affected by osteoarthritis or primary fibromyalgia syndrome were also investigated for serum markers of fibroblast (carboxyterminal propeptide of collagen I), endothelial (soluble E-selectin) and T-cell (soluble IL-2 receptor alpha) activation. RESULTS: Thirty-two of the 71 patients (45.1%) had both a marker autoantibody and a capillaroscopic scleroderma pattern (subset 1), 16 patients (22.5%) had only a marker autoantibody (subset 2), and 23 patients (32.4%) had only a capillaroscopic scleroderma pattern (subset 3). Patients with marker autoantibodies (n = 48, 67.6%) had a higher prevalence of impaired diffusing lung capacity for carbon monoxide (P = 0.0217) and increased serum levels of carboxyterminal propeptide of collagen I (P = 0.0037), regardless of capillaroscopic alterations. Patients with a capillaroscopic scleroderma pattern (n = 55, 77.5%) had a higher prevalence of puffy fingers (P = 0.0001) and increased serum levels of soluble E-selectin (P = 0.0003) regardless of marker autoantibodies. CONCLUSION: These results suggest that the autoantibody and microvascular patterns in early SSc may each be related to different clinical-preclinical features and circulating activation markers at presentation. Longitudinal studies are warranted to investigate whether these subsets undergo a different disease course over time. BioMed Central 2013 2013-05-29 /pmc/articles/PMC4060381/ /pubmed/23718566 http://dx.doi.org/10.1186/ar4236 Text en Copyright © 2013 Valentini et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Valentini, Gabriele
Marcoccia, Antonella
Cuomo, Giovanna
Vettori, Serena
Iudici, Michele
Bondanini, Francesco
Santoriello, Carlo
Ciani, Aldo
Cozzolino, Domenico
De Matteis, Giovanni Maria
Cappabianca, Salvatore
Vitelli, Filiberto
Spanò, Alberto
Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title_full Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title_fullStr Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title_full_unstemmed Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title_short Early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
title_sort early systemic sclerosis: marker autoantibodies and videocapillaroscopy patterns are each associated with distinct clinical, functional and cellular activation markers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4060381/
https://www.ncbi.nlm.nih.gov/pubmed/23718566
http://dx.doi.org/10.1186/ar4236
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