Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis

Inhalation of crystalline silica (SiO(2)) is a risk factor of systemic autoimmune diseases such as systemic sclerosis (SSc) and fibrotic pulmonary disorders such as silicosis. A defect of apoptotic cell clearance (i.e., efferocytosis, a key process in the resolution of inflammation) is reported in m...

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Autores principales: Lescoat, Alain, Ballerie, Alice, Lelong, Marie, Augagneur, Yu, Morzadec, Claudie, Jouneau, Stéphane, Jégo, Patrick, Fardel, Olivier, Vernhet, Laurent, Lecureur, Valérie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7039938/
https://www.ncbi.nlm.nih.gov/pubmed/32133004
http://dx.doi.org/10.3389/fimmu.2020.00219
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author Lescoat, Alain
Ballerie, Alice
Lelong, Marie
Augagneur, Yu
Morzadec, Claudie
Jouneau, Stéphane
Jégo, Patrick
Fardel, Olivier
Vernhet, Laurent
Lecureur, Valérie
author_facet Lescoat, Alain
Ballerie, Alice
Lelong, Marie
Augagneur, Yu
Morzadec, Claudie
Jouneau, Stéphane
Jégo, Patrick
Fardel, Olivier
Vernhet, Laurent
Lecureur, Valérie
author_sort Lescoat, Alain
collection PubMed
description Inhalation of crystalline silica (SiO(2)) is a risk factor of systemic autoimmune diseases such as systemic sclerosis (SSc) and fibrotic pulmonary disorders such as silicosis. A defect of apoptotic cell clearance (i.e., efferocytosis, a key process in the resolution of inflammation) is reported in macrophages from patients with fibrotic or autoimmune diseases. However, the precise links between SiO(2) exposure and efferocytosis impairment remain to be determined. Answering to this question may help to better link innate immunity and fibrosis. In this study, we first aim to determine whether SiO(2) might alter efferocytosis capacities of human and mouse macrophages. We secondly explore possible mechanisms explaining efferocytosis impairment, with a specific focus on macrophage polarization and on the RhoA/ROCK pathway, a key regulator of cytoskeleton remodeling and phagocytosis. Human monocyte-derived macrophages (MDM) and C57BL/6J mice exposed to SiO(2) and to CFSE-positive apoptotic Jurkat cells were analyzed by flow cytometry to determine their efferocytosis index (EI). The effects of ROCK inhibitors (Y27632 and Fasudil) on EI of SiO(2)-exposed MDM and MDM from SSc patients were evaluated in vitro. Our results demonstrated that SiO(2) significantly decreased EI of human MDM in vitro and mouse alveolar macrophages in vivo. In human MDM, this SiO(2)-associated impairment of efferocytosis, required the expression of the membrane receptor SR-B1 and was associated with a decreased expression of M2 polarization markers (CD206, CD204, and CD163). F-actin staining, RhoA activation and impairment of efferocytosis, all induced by SiO(2), were reversed by ROCK inhibitors. Moreover, the EI of MDM from SSc patients was similar to the EI of in vitro- SiO(2)-exposed MDM and Y27632 significantly increased SSc MDM efferocytosis capacities, suggesting a likewise activation of the RhoA/ROCK pathway in SSc. Altogether, our results demonstrate that SiO(2) exposure may contribute to the impairment of efferocytosis capacities of mouse and human macrophages but also of MDM in SiO(2)-associated autoimmune diseases and fibrotic disorders such as SSc; in this context, the silica/RhoA/ROCK pathway may constitute a relevant therapeutic target.
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spelling pubmed-70399382020-03-04 Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis Lescoat, Alain Ballerie, Alice Lelong, Marie Augagneur, Yu Morzadec, Claudie Jouneau, Stéphane Jégo, Patrick Fardel, Olivier Vernhet, Laurent Lecureur, Valérie Front Immunol Immunology Inhalation of crystalline silica (SiO(2)) is a risk factor of systemic autoimmune diseases such as systemic sclerosis (SSc) and fibrotic pulmonary disorders such as silicosis. A defect of apoptotic cell clearance (i.e., efferocytosis, a key process in the resolution of inflammation) is reported in macrophages from patients with fibrotic or autoimmune diseases. However, the precise links between SiO(2) exposure and efferocytosis impairment remain to be determined. Answering to this question may help to better link innate immunity and fibrosis. In this study, we first aim to determine whether SiO(2) might alter efferocytosis capacities of human and mouse macrophages. We secondly explore possible mechanisms explaining efferocytosis impairment, with a specific focus on macrophage polarization and on the RhoA/ROCK pathway, a key regulator of cytoskeleton remodeling and phagocytosis. Human monocyte-derived macrophages (MDM) and C57BL/6J mice exposed to SiO(2) and to CFSE-positive apoptotic Jurkat cells were analyzed by flow cytometry to determine their efferocytosis index (EI). The effects of ROCK inhibitors (Y27632 and Fasudil) on EI of SiO(2)-exposed MDM and MDM from SSc patients were evaluated in vitro. Our results demonstrated that SiO(2) significantly decreased EI of human MDM in vitro and mouse alveolar macrophages in vivo. In human MDM, this SiO(2)-associated impairment of efferocytosis, required the expression of the membrane receptor SR-B1 and was associated with a decreased expression of M2 polarization markers (CD206, CD204, and CD163). F-actin staining, RhoA activation and impairment of efferocytosis, all induced by SiO(2), were reversed by ROCK inhibitors. Moreover, the EI of MDM from SSc patients was similar to the EI of in vitro- SiO(2)-exposed MDM and Y27632 significantly increased SSc MDM efferocytosis capacities, suggesting a likewise activation of the RhoA/ROCK pathway in SSc. Altogether, our results demonstrate that SiO(2) exposure may contribute to the impairment of efferocytosis capacities of mouse and human macrophages but also of MDM in SiO(2)-associated autoimmune diseases and fibrotic disorders such as SSc; in this context, the silica/RhoA/ROCK pathway may constitute a relevant therapeutic target. Frontiers Media S.A. 2020-02-18 /pmc/articles/PMC7039938/ /pubmed/32133004 http://dx.doi.org/10.3389/fimmu.2020.00219 Text en Copyright © 2020 Lescoat, Ballerie, Lelong, Augagneur, Morzadec, Jouneau, Jégo, Fardel, Vernhet and Lecureur. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Lescoat, Alain
Ballerie, Alice
Lelong, Marie
Augagneur, Yu
Morzadec, Claudie
Jouneau, Stéphane
Jégo, Patrick
Fardel, Olivier
Vernhet, Laurent
Lecureur, Valérie
Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title_full Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title_fullStr Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title_full_unstemmed Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title_short Crystalline Silica Impairs Efferocytosis Abilities of Human and Mouse Macrophages: Implication for Silica-Associated Systemic Sclerosis
title_sort crystalline silica impairs efferocytosis abilities of human and mouse macrophages: implication for silica-associated systemic sclerosis
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7039938/
https://www.ncbi.nlm.nih.gov/pubmed/32133004
http://dx.doi.org/10.3389/fimmu.2020.00219
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