eLife (May 2021)

Tendon and motor phenotypes in the Crtap-/- mouse model of recessive osteogenesis imperfecta

  • Matthew William Grol,
  • Nele A Haelterman,
  • Joohyun Lim,
  • Elda M Munivez,
  • Marilyn Archer,
  • David M Hudson,
  • Sara F Tufa,
  • Douglas R Keene,
  • Kevin Lei,
  • Dongsu Park,
  • Cole D Kuzawa,
  • Catherine G Ambrose,
  • David R Eyre,
  • Brendan H Lee

DOI
https://doi.org/10.7554/eLife.63488
Journal volume & issue
Vol. 10

Abstract

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Osteogenesis imperfecta (OI) is characterized by short stature, skeletal deformities, low bone mass, and motor deficits. A subset of OI patients also present with joint hypermobility; however, the role of tendon dysfunction in OI pathogenesis is largely unknown. Using the Crtap-/- mouse model of severe, recessive OI, we found that mutant Achilles and patellar tendons were thinner and weaker with increased collagen cross-links and reduced collagen fibril size at 1- and 4-months compared to wildtype. Patellar tendons from Crtap-/- mice also had altered numbers of CD146+CD200+ and CD146-CD200+ progenitor-like cells at skeletal maturity. RNA-seq analysis of Achilles and patellar tendons from 1-month Crtap-/- mice revealed dysregulation in matrix and tendon marker gene expression concomitant with predicted alterations in TGF-β, inflammatory, and metabolic signaling. At 4-months, Crtap-/- mice showed increased αSMA, MMP2, and phospho-NFκB staining in the patellar tendon consistent with excess matrix remodeling and tissue inflammation. Finally, a series of behavioral tests showed severe motor impairments and reduced grip strength in 4-month Crtap-/- mice – a phenotype that correlates with the tendon pathology.

Keywords