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Acta neuropathologica communications
Jul 01, 2013;1 29.

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

Annie Hiniker, Brianne H Daniels, Han S Lee, Marta Margeta
Author Information
  1. Annie Hiniker: Department of Pathology, University of California San Francisco, San Francisco, CA 94143, USA. Marta.Margeta@ucsf.edu.
PMID: 24252466 DOI: 10.1186/2051-5960-1-29

Abstract

BACKGROUND: 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.
RESULTS: We performed quantitative immunohistochemistry for (1) autophagic markers LC3 and p62 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 LC3 and p62 were sensitive markers of IBM, but the tradeoff between sensitivity and specificity was smaller (and diagnostic utility thus greater) for LC3 than for p62. 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.
CONCLUSIONS: To differentiate IBM from PM, we thus recommend using a panel of LC3 and TDP-43 antibodies: the finding of <14% LC3-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.

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MeSH Term

Adult
Aged
Aged, 80 and over
Biomarkers
Creatine Kinase
DNA-Binding Proteins
Diagnosis, Differential
Female
Humans
Immunohistochemistry
Male
Microtubule-Associated Proteins
Middle Aged
Muscles
Myositis
Myositis, Inclusion Body
Polymyositis
RNA-Binding Proteins
Sensitivity and Specificity
Tissue Fixation

Chemicals

Biomarkers
DNA-Binding Proteins
MAP1LC3A protein, human
Microtubule-Associated Proteins
P62 protein, human
RNA-Binding Proteins
Creatine Kinase
Comparative Study Journal Article
Article has an altmetric score of 1

Word Cloud

Created with Highcharts 10.0.0IBMPMLC3p62TDP-43fibersinflammatorypolymyositismarkerssensitivitybodymyositisshowtwoimmunohistochemistryproteinaggregationmyopathiesspecificityutilitythusBACKGROUND:InclusionslowlyprogressivemyopathyelderlysignificantclinicalimprovementresponsesteroidtherapyDistinguishingclinicallyimportantsincesteroid-responsivehoweverconditionscansubstantialhistologicoverlapRESULTS:performedquantitative1autophagic2marker53subjectspathologicallydiagnosedintermediateTcell-mediatedCOX-negativepossiblepercentagestainedsignificantlyhigherthreeimmunostainsvariedparticularsensitivetradeoffsmallerdiagnosticgreatercontrastimmunopositivityhighlyspecifictestlowdefinitivestainingpresentjust67%casesCONCLUSIONS:differentiaterecommendusingpanelantibodies:finding<14%LC3-positivehelpsexclude>7%TDP-43-positivestronglysupportsdiagnosisdataprovidesupporthypothesisdisruptionautophagycontributepathogenesisComparativedifferentiationinclusionrelated

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