Th1 response and systemic treg deficiency in inclusion body myositis.

[inclusion body myositis]

Sporadic inclusion body myositis (sIBM ), the most frequent myositis in elderly patients , is characterized by the presence muscle inflammation and degeneration . We aimed at characterizing immune responses and regulatory T cells , considered key players in the maintenance of peripheral immune tolerance , in sIBM .Serum and muscle tissue levels of 25 cytokines and phenotype of circulating immune cells were measured in 22 sIBM patients and compared with 22 healthy subjects . Cytokine data were analysed by unsupervised hierarchical clustering and principal components analysis .Compared to healthy controls , sIBM patients had increased levels of Th-1 cytokines and chemokines such as IL -12 (261 ±138 pg /mL vs . 88 ±19 pg /mL ; p <0 .0001 ), CXCL-9 (186 ±12 pg /mL vs . 13 ±7 pg /mL ; p <0 .0001 ), and CXCL-10 (187 ±62 pg /mL vs . 13 ±6 pg /mL ; p <0 .0001 ). This was associated with an increased frequency of CD 8 +CD 28 - T cells (45 .6 ±18 .5 % vs . 13 .5 ±9 .9 %; p <0 .0001 ), which were more prone to produce IFN-γ (45 .6 ±18 .5 % vs . 13 .5 ±9 .9 %; p <0 .0001 ). sIBM patients also had a decreased frequency of circulating regulatory T cells (CD 4 +CD 2 5 +CD 127 lowFOXP 3 +, 6 .9 ±1 .7 %; vs . 5 .2 ±1 .1 %, p = 0 .01 ), which displayed normal suppressor function and were also present in affected muscle .sIBM patients present systemic immune activation with Th 1 polarization involving the IFN-γ pathway and CD 8 +CD 28 - T cells associated with peripheral regulatory T cell deficiency .