| Literature DB >> 29741608 |
Leandro Ladislau1,2, Xavier Suárez-Calvet1,3,4, Ségolène Toquet1, Océane Landon-Cardinal1, Damien Amelin1, Marine Depp5, Mathieu P Rodero5, Denisa Hathazi6, Darragh Duffy7, Vincent Bondet7, Corinna Preusse8, Boris Bienvenu9, Flore Rozenberg10, Andreas Roos6,11, Claudia F Benjamim2, Eduard Gallardo3,4, Isabel Illa3,4, Vincent Mouly1, Werner Stenzel8, Gillian Butler-Browne1, Olivier Benveniste1, Yves Allenbach1.
Abstract
Dermatomyositis is an acquired auto-immune disease characterized by skin lesions and muscle-specific pathological features such as perifascicular muscle fibre atrophy and vasculopathy. Dermatomyositis patients display an upregulation of type I interferon-inducible genes in muscle fibres, endothelial cells, skin and peripheral blood. However, the effect of type I interferon on muscle tissue has not yet been determined. Our aim was to study the pathogenicity of type I interferon in vitro and to evaluate the efficacy of the type I interferon pathway blockade for therapeutic purposes. The activation of type I interferon in differentiating myoblasts abolished myotube formation with reduced myogenin expression while in differentiated myotubes, we observed a reduction in surface area and an upregulation of atrophy-associated genes. In vitro endothelial cells exposure to type I interferon disrupted vascular network organization. All the pathogenic effects observed in vitro were abolished by ruxolitinib. Finally, four refractory dermatomyositis patients were treated with ruxolitinib and improvement ensued in skin lesions, muscle weakness and a reduced serum type I interferon levels and interferon-inducbile genes scores. We propose JAK inhibition as a mechanism-based treatment for dermatomyositis, a finding that is relevant for the design of future clinical trials targeting dermatomyositis.Entities:
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Year: 2018 PMID: 29741608 DOI: 10.1093/brain/awy105
Source DB: PubMed Journal: Brain ISSN: 0006-8950 Impact factor: 13.501