Increased IL-15 production of muscle cells in polymyositis and dermatomyositis

doi:10.1093/intimm/dxf062

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International Immunology, Vol. 14, No. 8, pp. 917-924, August 2002
© 2002 Japanese Society for Immunology

Increased IL-15 production of muscle cells in polymyositis and dermatomyositis

Tomoko Sugiura¹, Masayoshi Harigai¹, Yasushi Kawaguchi¹, Kae Takagi¹, Chikako Fukasawa¹, Satomi Ohsako-Higami¹, Shuji Ohta¹, Michi Tanaka¹, Masako Hara¹ and Naoyuki Kamatani¹

¹ Institute of Rheumatology, Tokyo Women’s Medical University, 10-22 Kawada-cho, Shinjuku-ku, Tokyo 162-0054, Japan

Correspondence to: T. Sugiura; E-mail: tsugiura{at}ior.twmu.ac.jp
Transmitting editor: T. Watanabe

In polymyositis (PM)/dermatomyositis (DM), various cytokines,especially macrophage-derived cytokines such as IL-1 ${alpha}$ , IL-1ßand tumor necrosis factor (TNF)- ${alpha}$ , are expressed in the inflammatoryfoci. We previously reported that IL-15, a novel cytokine witha biological activity similar to that of IL-2, is expressedin muscle cells in PM/DM. In the present study, we set out toinvestigate the regulation of IL-15 in cultured myoblasts. Myoblastsconstitutively produced a low level of IL-15 and the productionwas augmented by stimulation with IFN- ${gamma}$ , IL-1 ${alpha}$ , IL-1ß,TNF- ${alpha}$ or lipopolysaccharide (LPS) in a dose-dependent manner.These stimuli also enhanced the expression of IL-15 mRNA. About30–40% of IL-15 was detected intracellularly, while therest was released into the culture supernatant. Immunohistochemicalstaining revealed that intracellular IL-15 was localized inthe perinuclear area of the cytoplasm in the myoblasts. Despitethe considerable amounts of intracellular IL-15, the myoblastspredominantly expressed authentic IL-15 mRNA isoform. This isoformgenerates IL-15 with long signal peptide preprotein, which isall to be secreted. The biological activity of IL-15 secretedfrom the myoblasts was examined using an IL-15-dependent murineT cell line, CTLL-2. Culture supernatants of the myoblasts induceda proliferative response of CTLL-2 and this was specificallyinhibited by anti-IL-15 antibody. These results suggest thatinflammatory stimuli induce the production of IL-15 in the musclecells in PM/DM, and IL-15 may contribute to the immunopathogenesisby augmenting recruitment and activation of the infiltratingT cells. Blocking of IL-15 production might be of therapeuticvalue in PM/DM.

Keywords: dermatomyositis, IL-15, muscle cells, polymyositis

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