4.6 Article

Increased skeletal muscle-specific microRNA in the blood of patients with COPD

Journal

THORAX
Volume 68, Issue 12, Pages 1140-1149

Publisher

BMJ PUBLISHING GROUP
DOI: 10.1136/thoraxjnl-2012-203129

Keywords

COPD Pathology; Exercise; Systemic disease and lungs

Funding

  1. NIHR Respiratory Disease Biomedical Research Unit at the Royal Brompton
  2. Harefield NHS Foundation Trust
  3. Imperial College London
  4. COPD-MAP
  5. NIHR
  6. BBSRC [BB/H530703/1]
  7. MRC [COPD-MAP G1001362]
  8. BBSRC [BB/H530703/1] Funding Source: UKRI
  9. MRC [G1002113] Funding Source: UKRI
  10. Medical Research Council [G1002113] Funding Source: researchfish
  11. National Institute for Health Research [DHCS/07/07/009, CTF-01-12-04] Funding Source: researchfish

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Background Skeletal muscle weakness in chronic obstructive pulmonary disease (COPD) carries a poor prognosis, therefore a non-invasive marker of this process could be useful. Reduced expression of muscle-specific microRNA (myomiRs) in quadriceps muscle in patients with COPD is associated with skeletal muscle weakness and changes in muscle fibre composition. Circulating exosomal miRNAs can be measured in blood, making them candidate biomarkers of biopsy phenotype. To determine whether plasma myomiR levels were associated with fibre size or fibre proportion, we measured myomiRs in plasma from patients with COPD and healthy controls. Methods and results 103 patients with COPD and 25 age-matched controls were studied. Muscle-specific miRNA was elevated in the plasma of patients with COPD and showed distinct patterns. Specifically, miR-1 was inversely associated with fat-free mass in the cohort, whereas levels of miR-499 were more directly associated with strength and quadriceps type I fibre proportion. Two miRs not restricted to muscle in origin (miR-16 and miR-122) did not differ between patients and controls. Plasma miR-499 was also associated with muscle nuclear factor B p50 but not p65 in patients with early COPD whereas plasma inflammatory cytokines were associated with miR-206 in patients with more advanced disease. Conclusions Plasma levels of individual myomiRs are altered in patients with COPD but alone do not predict muscle fibre size or proportion. Our findings are consistent with an increase in muscle wasting and turnover associated with the development of skeletal muscle dysfunction and fibre-type shift in patients with stable COPD.

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