Comparative utility of LC3, p62 and TDP-43 immunohistochemistry in differentiation of inclusion body myositis from polymyositis and related inflammatory myopathies.

[inclusion body myositis]

Inclusion body myositis (IBM ) is a slowly progressive inflammatory myopathy of the elderly that does not show significant clinical improvement in response to steroid therapy . Distinguishing IBM from polymyositis (PM ) is clinically important since PM is steroid-responsive ; however , the two conditions can show substantial histologic overlap .We performed quantitative immunohistochemistry for (1 ) autophagic markers LC 3 and p 62 and (2 ) protein aggregation marker TDP-43 in 53 subjects with pathologically diagnosed PM , IBM , and two intermediate T cell-mediated inflammatory myopathies (polymyositis with COX -negative fibers and possible IBM ). The percentage of stained fibers was significantly higher in IBM than PM for all three immunostains , but the markers varied in sensitivity and specificity . In particular , both LC 3 and p 62 were sensitive markers of IBM , but the tradeoff between sensitivity and specificity was smaller (and diagnostic utility thus greater ) for LC 3 than for p 62 . In contrast , TDP-43 immunopositivity was highly specific for IBM , but the sensitivity of this test was low , with definitive staining present in just 67 % of IBM cases .To differentiate IBM from PM , we thus recommend using a panel of LC 3 and TDP-43 antibodies : the finding of <14 % LC 3 -positive fibers helps exclude IBM , while >7 % of TDP-43 -positive fibers strongly supports a diagnosis of IBM . These data provide support for the hypothesis that disruption of autophagy and protein aggregation contribute to IBM pathogenesis .