Intestinal decontamination inhibits TLR4 dependent fibronectin-mediated cross-talk between stellate cells and endothelial cells in liver fibrosis in mice

Zhu, Qiang; Zou, Li; Jagavelu, Kumaravelu; Simonetto, Douglas A.; Huebert, Robert C.; Jiang, Zhi-Dong; DuPont, Herbert L.; Shah, Vijay H.

doi:10.1016/j.jhep.2011.11.013

« Previous Next »Journal of Hepatology
Volume 56, Issue 4 , Pages 893-899, April 2012

Intestinal decontamination inhibits TLR4 dependent fibronectin-mediated cross-talk between stellate cells and endothelial cells in liver fibrosis in mice

Qiang Zhu
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
- Provincial Hospital Affiliated to Shandong University, Ji’nan, China
- The authors contributed equally to this work.
Li Zou
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
- The authors contributed equally to this work.
Kumaravelu Jagavelu
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
Douglas A. Simonetto
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
Robert C. Huebert
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
Zhi-Dong Jiang
- University of Texas School of Public Health, Houston, TX, USA
Herbert L. DuPont
- University of Texas School of Public Health, Houston, TX, USA
Vijay H. Shah
- Gastroenterology Research Unit, Mayo Clinic and Foundation, Rochester, MN, USA
- Corresponding author. Address: Gastroenterology Research Unit, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA.

Received 21 June 2011; received in revised form 26 October 2011; accepted 3 November 2011. published online 14 December 2011.

Background & Aims

Liver fibrosis is associated with angiogenesis and leads to portal hypertension. Certain antibiotics reduce complications of liver failure in humans, however, the effects of antibiotics on the pathologic alterations of the disease are not fully understood. The aim of this study was to test whether the non-absorbable antibiotic rifaximin could attenuate fibrosis progression and portal hypertension in vivo, and explore potential mechanisms in vitro.

Methods

The effect of rifaximin on portal pressure, fibrosis, and angiogenesis was examined in wild type and Toll-like receptor 4 (TLR4) mutant mice after bile duct ligation (BDL). In vitro studies were carried out to evaluate the effect of the bacterial product and TLR agonist lipopolysaccharide (LPS) on paracrine interactions between hepatic stellate cells (HSC) and liver endothelial cells (LEC) that lead to fibrosis and portal hypertension.

Results

Portal pressure, fibrosis, and angiogenesis were significantly lower in BDL mice receiving rifaximin compared to BDL mice receiving vehicle. Studies in TLR4 mutant mice confirmed that the effect of rifaximin was dependent on LPS/TLR4 pathway. Fibronectin (FN) was increased in the BDL liver and was reduced by rifaximin administration and thus, was explored further in vitro as a potential mediator of paracrine interactions of HSC and LEC. In vitro, LPS promoted FN production from HSC. Furthermore, HSC-derived FN promoted LEC migration and angiogenesis.

Conclusions

These studies expand our understanding of the relationship of intestinal microbiota with fibrosis development by identifying FN as a TLR4 dependent mediator of the matrix and vascular changes that characterize cirrhosis.

Abbreviations: LPS, lipopolysaccharide, TLR4, Toll-like receptor-4, LEC, liver endothelial cells, HSC, hepatic stellate cells, FN, fibronectin, BDL, bile duct ligation, LPSBP, lipopolysaccharide binding protein, vWF, von Willebrand’s factor, PDGFR-β, platelet-derived growth factor receptor-β