PLoS ONE (Jan 2008)

BMP-7 does not protect against bleomycin-induced lung or skin fibrosis.

  • Lynne A Murray,
  • Tillie L Hackett,
  • Stephanie M Warner,
  • Furquan Shaheen,
  • Rochelle L Argentieri,
  • Paul Dudas,
  • Francis X Farrell,
  • Darryl A Knight

DOI
https://doi.org/10.1371/journal.pone.0004039
Journal volume & issue
Vol. 3, no. 12
p. e4039

Abstract

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Bone morphogenic protein (BMP)-7 is a member of the BMP family which are structurally and functionally related, and part of the TGFbeta super family of growth factors. BMP-7 has been reported to inhibit renal fibrosis and TGFbeta1-induced epithelial-mesenchymal transition (EMT), in part through negative interactions with TGFbeta1 induced Smad 2/3 activation. We utilized in vivo bleomycin-induced fibrosis models in the skin and lung to determine the potential therapeutic effect of BMP-7. We then determined the effect of BMP-7 on TGFbeta1-induced EMT in lung epithelial cells and collagen production by human lung fibroblasts. We show that BMP-7 did not affect bleomycin-induced fibrosis in either the lung or skin in vivo; had no effect on expression of pro-fibrotic genes by human lung fibroblasts, either at rest or following exposure to TGFbeta1; and did not modulate TGFbeta1-induced EMT in human lung epithelial cells. Taken together our data indicates that BMP-7 has no anti-fibrotic effect in lung or skin fibrosis either in vivo or in vitro. This suggests that the therapeutic options for BMP-7 may be confined to the renal compartment.