PLoS ONE (Jan 2014)

Inflammation-induced acute phase response in skeletal muscle and critical illness myopathy.

  • Claudia Langhans,
  • Steffen Weber-Carstens,
  • Franziska Schmidt,
  • Jida Hamati,
  • Melanie Kny,
  • Xiaoxi Zhu,
  • Tobias Wollersheim,
  • Susanne Koch,
  • Martin Krebs,
  • Herbert Schulz,
  • Doerte Lodka,
  • Kathrin Saar,
  • Siegfried Labeit,
  • Claudia Spies,
  • Norbert Hubner,
  • Joachim Spranger,
  • Simone Spuler,
  • Michael Boschmann,
  • Gunnar Dittmar,
  • Gillian Butler-Browne,
  • Vincent Mouly,
  • Jens Fielitz

DOI
https://doi.org/10.1371/journal.pone.0092048
Journal volume & issue
Vol. 9, no. 3
p. e92048

Abstract

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ObjectivesSystemic inflammation is a major risk factor for critical-illness myopathy (CIM) but its pathogenic role in muscle is uncertain. We observed that interleukin 6 (IL-6) and serum amyloid A1 (SAA1) expression was upregulated in muscle of critically ill patients. To test the relevance of these responses we assessed inflammation and acute-phase response at early and late time points in muscle of patients at risk for CIM.DesignProspective observational clinical study and prospective animal trial.SettingTwo intensive care units (ICU) and research laboratory.Patients/subjects33 patients with Sequential Organ Failure Assessment scores ≥ 8 on 3 consecutive days within 5 days in ICU were investigated. A subgroup analysis of 12 patients with, and 18 patients without CIM (non-CIM) was performed. Two consecutive biopsies from vastus lateralis were obtained at median days 5 and 15, early and late time points. Controls were 5 healthy subjects undergoing elective orthopedic surgery. A septic mouse model and cultured myoblasts were used for mechanistic analyses.Measurements and main resultsEarly SAA1 expression was significantly higher in skeletal muscle of CIM compared to non-CIM patients. Immunohistochemistry showed SAA1 accumulations in muscle of CIM patients at the early time point, which resolved later. SAA1 expression was induced by IL-6 and tumor necrosis factor-alpha in human and mouse myocytes in vitro. Inflammation-induced muscular SAA1 accumulation was reproduced in a sepsis mouse model.ConclusionsSkeletal muscle contributes to general inflammation and acute-phase response in CIM patients. Muscular SAA1 could be important for CIM pathogenesis.Trial registrationISRCTN77569430.