Hepatocyte-Specific Smad7 Expression Attenuates TGF-β–Mediated Fibrogenesis and Protects Against Liver Damage

Abstract: The data indicate that hepatocytes undergo TGF-beta-dependent EMT-like phenotypic changes and actively participate in fibrogenesis. Furthermore, ablation of TGF-beta signaling specifically in this cell type is sufficient to blunt the fibrogenic response.

“…5% of the hepatic cells were coexpressing either FSP-1 and albumin or FSP-1 and β-gal, then suggestive of EMT. Moreover, in the same study the treatment with bone morphogenetic protein-7 (BMP-7), which is known to antagonize TGFβ1 signaling, significantly inhibited liver fibrosis and almost abolished putative EMT-derived fibroblasts/MFs, a result also obtained by another laboratory using transgenic mouse over-expressing Smad7 in hepatocytes [26]. The latter study also reported some morphological evidence for "in vivo" EMT in biopsies from chronic HBV patients.…”

Cellular and molecular mechanisms in liver fibrogenesis

“…5% of the hepatic cells were coexpressing either FSP-1 and albumin or FSP-1 and β-gal, then suggestive of EMT. Moreover, in the same study the treatment with bone morphogenetic protein-7 (BMP-7), which is known to antagonize TGFβ1 signaling, significantly inhibited liver fibrosis and almost abolished putative EMT-derived fibroblasts/MFs, a result also obtained by another laboratory using transgenic mouse over-expressing Smad7 in hepatocytes [26]. The latter study also reported some morphological evidence for "in vivo" EMT in biopsies from chronic HBV patients.…”

Cellular and molecular mechanisms in liver fibrogenesis

“…Given the prominent role of TGFb in EMT and fibrogenesis, a number of strategies for blocking TGF-b signaling have been proposed. [22][23][24] Small molecules targeting this signaling cascade have great therapeutic potential. To identify such candidates, a drug library screen was performed using (CAGA) 12 -Lux, a luciferase reporter that is activated in response to a wide range of TGF-b1 concentrations (Supporting Fig.…”

“…27 To date, this cell line has been used extensively as an ideal model to assess TGF-b-induced EMT on the resultant cellular phenotypes and gene expression profiles in vitro. 8,18,24 When exposed to TGF-b1 for 48 hours, AML12 cells underwent EMT, in which cells lost their epithelial honeycomb-like morphology and obtained a spindle-like shape ( Fig. 2A).…”

“…22,23 Similarly, ectopic overexpression of Smad7 in the hepatocytes of transgenic mice was shown to attenuate TGF-b signaling and thereby improve CCl 4 -induced liver fibrosis. 24 In addition to these protein-based therapies, small molecules and biological agents that act on this signaling cascade have shown strong therapeutic potential in clinical settings. However, efficient and well-tolerated antifibrotic drugs are currently lacking.…”

Sorafenib inhibits transforming growth factor β1-Mediated Epithelial-Mesenchymal Transition and apoptosis in mouse hepatocytes

“…TGF-β1 signaling participates in various physiological and pathological processes including embryonic development, tissue differentiation, cell proliferation, inflammation, angiogenesis, tumorigenesis as well as fibrosis (Wu et al 2016;Lei et al 2017;Li et al 2017;Tang et al 2017;Wang et al 2017;Yamazaki et al 2017;Yang et al 2017). Through regulating Smad2/3, TGF-β1 modulates the transcription and expression of several fibrosis-associated genes, thereby enhancing the synthesis of collagen and fibronectin (Dooley et al 2008;Yan and Chen 2011;Massague 2012). Overstimulation of TGF-β signaling pathway contributes to aberrant deposition of extracellular matrix (ECM), leading to the pathological heart remodeling after AMI (Dobaczewski et al 2011).…”

Exogenous BMP-7 Facilitates the Recovery of Cardiac Function after Acute Myocardial Infarction through Counteracting TGF-<i>β</i>1 Signaling Pathway