Osteopontin promotes fibrosis in dystrophic mouse muscle by modulating immune cell subsets and intramuscular TGF-β
Sylvia A. Vetrone, Encarnacion Montecino-Rodriguez, Elena Kudryashova, Irina Kramerova, Eric P. Hoffman, Scot D. Liu, M. Carrie Miceli, Melissa J. Spencer
Sylvia A. Vetrone, Encarnacion Montecino-Rodriguez, Elena Kudryashova, Irina Kramerova, Eric P. Hoffman, Scot D. Liu, M. Carrie Miceli, Melissa J. Spencer
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Research Article Muscle biology

Osteopontin promotes fibrosis in dystrophic mouse muscle by modulating immune cell subsets and intramuscular TGF-β

Abstract

Duchenne muscular dystrophy (DMD) is an X-linked, degenerative muscle disease that is exacerbated by secondary inflammation. Here, we characterized the immunological milieu of dystrophic muscle in mdx mice, a model of DMD, to identify potential therapeutic targets. We identified a specific subpopulation of cells expressing the Vβ8.1/8.2 TCR that is predominant among TCR-β+ T cells. These cells expressed high levels of osteopontin (OPN), a cytokine that promotes immune cell migration and survival. Elevated OPN levels correlated with the dystrophic process, since OPN was substantially elevated in the serum of mdx mice and muscle biopsies after disease onset. Muscle biopsies from individuals with DMD also had elevated OPN levels. To test the role of OPN in mdx muscle, mice lacking both OPN and dystrophin were generated and termed double-mutant mice (DMM mice). Reduced infiltration of NKT-like cells and neutrophils was observed in the muscle of DMM mice, supporting an immunomodulatory role for OPN in mdx muscle. Concomitantly, an increase in CD4+ and FoxP3+ Tregs was also observed in DMM muscle, which also showed reduced levels of TGF-β, a known fibrosis mediator. These inflammatory changes correlated with increased strength and reduced diaphragm and cardiac fibrosis. These studies suggest that OPN may be a promising therapeutic target for reducing inflammation and fibrosis in individuals with DMD.

Authors

Sylvia A. Vetrone, Encarnacion Montecino-Rodriguez, Elena Kudryashova, Irina Kramerova, Eric P. Hoffman, Scot D. Liu, M. Carrie Miceli, Melissa J. Spencer

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Figure 5

Ablation of OPN leads to changes in intramuscular inflammatory cells.

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Ablation of OPN leads to changes in intramuscular inflammatory cells. In...
Infiltrating leukocytes were isolated from mdx and DMM mice and characterized by flow cytometry as described in Methods. Each experiment was performed on leukocytes isolated from muscles of 4 grouped 4-week-old mdx or DMM mice, which were stained for cell surface markers and analyzed by flow cytometry. Data represent the percentage difference in DMM muscles of intramuscular inflammatory cells bearing the indicated cell surface markers compared with mdx muscles. Data were assessed from 6–8 experiments per stain. *P ≤ 0.05, **P ≤ 0.01, as assessed by Mann-Whitney U test (top panel). Cross sections of 6-month-old mdx and DMM diaphragm muscles immunostained for Ly6G, a neutrophil marker (red) and counterstained for hematoxylin (blue). Original magnification of ×20 (bottom panel).