Mesenchymal stromal cell exosomes prevent and revert experimental pulmonary fibrosis through modulation of monocyte phenotypes
Nahal Mansouri, Gareth R. Willis, Angeles Fernandez-Gonzalez, Monica Reis, Sina Nassiri, S. Alex Mitsialis, Stella Kourembanas
Nahal Mansouri, Gareth R. Willis, Angeles Fernandez-Gonzalez, Monica Reis, Sina Nassiri, S. Alex Mitsialis, Stella Kourembanas
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Research Article Pulmonology Stem cells

Mesenchymal stromal cell exosomes prevent and revert experimental pulmonary fibrosis through modulation of monocyte phenotypes

Abstract

Mesenchymal stromal/stem cell (MSC) therapy has shown promise in experimental models of idiopathic pulmonary fibrosis (IPF). The aim of this study was to test the therapeutic effects of extracellular vesicles produced by human BM MSCs (MEx) in a bleomycin-induced pulmonary fibrosis model and investigate mechanisms of action. Adult C57BL/6 mice were challenged with endotracheal instillation of bleomycin and treated with MEx concurrently, or for reversal models, at day 7 or 21. Experimental groups were assessed at day 7, 14, or 28. Bleomycin-challenged mice presented with severe septal thickening and prominent fibrosis, and this was effectively prevented or reversed by MEx treatment. MEx modulated lung macrophage phenotypes, shifting the proportions of lung proinflammatory/classical and nonclassical monocytes and alveolar macrophages toward the monocyte/macrophage profiles of control mice. A parallel immunomodulatory effect was demonstrated in the BM. Notably, transplantation of MEx-preconditioned BM-derived monocytes alleviated core features of pulmonary fibrosis and lung inflammation. Proteomic analysis revealed that MEx therapy promotes an immunoregulatory, antiinflammatory monocyte phenotype. We conclude that MEx prevent and revert core features of bleomycin-induced pulmonary fibrosis and that the beneficial actions of MEx may be mediated via systemic modulation of monocyte phenotypes.

Authors

Nahal Mansouri, Gareth R. Willis, Angeles Fernandez-Gonzalez, Monica Reis, Sina Nassiri, S. Alex Mitsialis, Stella Kourembanas

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Figure 4

MEx therapy modulates alveolar macrophage and monocyte populations in the lung.

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MEx therapy modulates alveolar macrophage and monocyte populations in th...
(A and B) Flow cytometry was used to assess whole lung monocyte and alveolar macrophage (alveolar MΦ) at day 7 (A) and day 14 (B). (C) Classical monocytes (Mo) were defined as CD45+CD11b+MHCIICD64CCR-2+Ly6Chi. Nonclassical monocytes were defined as CD45+CD11b+MHCIICD64CCR-2Ly6Clo. Representative gating strategy of alveolar MΦ (CD45+ CD11b CD11c+ CD64+ cells), classical Mo, and nonclassical Mo. The gating strategy was performed according to fluorescence minus one controls (Supplemental Figure 1). Data are representative of 3 independent experiments, mean ± SD, n = 4–5 per experimental group; each symbol represents 1 mouse. *P < 0.05; **P < 0.01; ***P < 0.001. One-way ANOVA followed by Fisher’s LSD post hoc analysis.