Inhibition of myogenic microRNAs 1, 133, and 206 by inflammatory cytokines links inflammation and muscle degeneration in adult inflammatory myopathies.

[inclusion body myositis]

The molecular basis of inflammatory myopathies such as dermatomyositis (DM ), polymyositis , and inclusion body myositis , which share the characteristics of chronic muscle inflammation and skeletal muscle wasting , are poorly understood . As such , effective targeted treatments for these diseases are lacking , resulting in critical unmet medical needs for these devastating diseases . The purpose of this study was to identify possible new targets for drug development by exploring the mechanism by which inflammation may play a role in the pathology of the inflammatory myopathies .We compared expression levels of inflammatory cytokines and microRNAs (miRNAs ) between muscle biopsy samples from patients with inflammatory myopathies and those from donors without myositis . In vitro human and mouse model systems were then used to characterize the role of these cytokines and microRNAs on myoblast-to -myocyte differentiation .We observed increased expression of inflammatory cytokines , including tumor necrosis factor α (TNF α ), interferon-α (IFN α ), IFN β , and interleukin-1 β , in different subtypes of inflammatory myopathies . We observed decreased expression of microRNA-1 (miR-1 ), miR-133 a , and miR-133 b in all of the inflammatory myopathy subtypes we evaluated , as well as decreased expression of miR-206 in DM ; these miRNAs are essential for adult skeletal muscle differentiation and maintenance . TNF α was significantly inversely correlated with decreased myogenic miRNA expression in the inflammatory myopathy subtypes . In mechanistic studies , TNF α inhibited the expression of myogenic miRNAs and suppressed the differentiation of C 2 C 12 myoblasts to myocytes /myotubes in an NF-κB-dependent manner . This block in differentiation by TNF α was relieved by overexpression of miR-1 , miR-206 , or miR-133 a /b .Taken together , these results provide a new mechanistic link between the action of proinflammatory cytokines and the degenerative pathology of inflammatory myopathies , and suggest therapeutic approaches for these diseases .