BMC Gastroenterology (Oct 2009)

Liver fibrosis secondary to bile duct injury: correlation of Smad7 with TGF-β and extracellular matrix proteins

  • Fafutis-Morris Mary,
  • Martínez-Abundis Ricardo,
  • Hernández-Hoyos Sebastián,
  • Vázquez-Del Mercado Mónica,
  • Hermosillo-Sandoval José M,
  • Pizano-Martínez Oscar,
  • Yañez-Sánchez Irinea,
  • Miranda-Díaz Alejandra,
  • del Pilar Alatorre-Carranza María,
  • Segura-Ortega Jorge,
  • Delgado-Rizo Vidal

DOI
https://doi.org/10.1186/1471-230X-9-81
Journal volume & issue
Vol. 9, no. 1
p. 81

Abstract

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Abstract Background Liver fibrosis is the result of continuous liver injury stemming from different etiological factors. Bile duct injury induces an altered expression of TGF-β, which has an important role in liver fibrosis because this cytokine induces the expression of target genes such as collagens, PAI-1, TIMPs, and others that lead to extracellular matrix deposition. Smad7 is the principal inhibitor that regulates the target gene transcription of the TGF-β signaling. The aim of the study was to determine whether Smad7 mRNA expression correlates with the gene expression of TGF-β, Col I, Col III, Col IV, or PAI-1 in liver fibrosis secondary to bile duct injury (BDI). Results Serum TGF-β concentration was higher in BDI patients (39 296 pg/ml) than in liver donors (9008 pg/ml). Morphometric analysis of liver sections showed 41.85% of tissue contained fibrotic deposits in BDI patients. mRNA expression of Smad7, Col I, and PAI-1 was also significantly higher (P Conclusion We found augmented serum concentration of TGF-β and an increase in the percentage of fibrotic tissue in the liver of BDI patients. Contrary to expected results, the 6-fold increase in Smad7 expression did not inhibit the expression of TGF-β, collagens, and PAI-1. We also observed greater expression of Col I and Col III mRNA in BDI patients and significant correlations between their expression and TGF-β concentration and Smad7 mRNA expression.