Glucocorticoids and 11β-HSD1 are major regulators of intramyocellular protein metabolism

Stuart Morgan, Zaki Hassan-Smith, Craig Doig, Mark Sherlock, Paul Stewart, Gareth Lavery

Research output: Contribution to journalArticlepeer-review

16 Citations (Scopus)
140 Downloads (Pure)

Abstract

Background: The adverse metabolic effects of prescribed and endogenous glucocorticoid excess, 'Cushing's syndrome', create a significant health burden. Whilst skeletal muscle atrophy and resultant myopathy is a clinical feature, the molecular mechanisms underpinning these changes are not fully defined.

Methods: We have characterised the impact of glucocorticoids upon key metabolic pathways and processes regulating muscle size and mass including: protein synthesis, protein degradation and myoblast proliferation in both murine C2C12 and human primary myotube cultures. Furthermore, we have investigated the role of pre-receptor modulation of glucocorticoid availability by 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) in these processes.

Results: Corticosterone decreased myotube area, decreased protein synthesis and increased protein degradation in murine myotubes. This was supported by decreased mRNA expression of IGF1, decreased activating phosphorylation of mTOR, decreased phosphorylation of 4E-BP1 and increased mRNA expression of key atrophy markers including: atrogin-1, FOXO3a, Mstn, MuRF1. These findings were endorsed in human primary myotubes where cortisol also decreased protein synthesis and increased protein degradation. The effects of 11-dehydrocorticosterone (in murine myotubes) and cortisone (in human myotubes) on protein metabolism were indistinguishable from that of corticosterone/cortisol treatments. Selective 11β-HSD1 inhibition blocked the decrease in protein synthesis, increased in protein degradation and reduction in myotube area induced by 11-dehydrocorticosterone/cortisone. Furthermore, corticosterone/cortisol, but not 11-dehydrocorticosterone/cortisone, decreased murine and human myoblast proliferative capacity.

Conclusion: Glucocorticoids are potent regulators of skeletal muscle protein homeostasis and myoblast proliferation. Our data underscores the potential use of selective 11β-HSD1 inhibitors to ameliorate muscle-wasting effects associated with glucocorticoid excess.
Original languageEnglish
Pages (from-to)277-286
JournalJournal of Endocrinology
Volume229
Issue number3
Early online date5 Apr 2016
DOIs
Publication statusPublished - 1 Jun 2016

Keywords

  • glucocorticoid
  • 11β-HSD1
  • protein metabolism
  • Cushing’s syndrome

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