HSC-specific inhibition of Rho-kinase reduces portal pressure in cirrhotic rats without major systemic effects

Sabine Klein; Marike Marjolijn Van Beuge; Michaela Granzow; Leonie Beljaars; Robert Schierwagen; Sibel Kilic; Iren Heidari; Sebastian Huss; Tilman Sauerbruch; Klaas Poelstra; Jonel Trebicka

doi:10.1016/j.jhep.2012.07.033

HSC-specific inhibition of Rho-kinase reduces portal pressure in cirrhotic rats without major systemic effects

J Hepatol. 2012 Dec;57(6):1220-7. doi: 10.1016/j.jhep.2012.07.033. Epub 2012 Aug 6.

Authors

Sabine Klein¹, Marike Marjolijn Van Beuge, Michaela Granzow, Leonie Beljaars, Robert Schierwagen, Sibel Kilic, Iren Heidari, Sebastian Huss, Tilman Sauerbruch, Klaas Poelstra, Jonel Trebicka

Affiliation

¹ Department of Internal Medicine I, University of Bonn, Sigmund-Freud Straße 25, D-53105 Bonn, Germany.

PMID: 22878469
DOI: 10.1016/j.jhep.2012.07.033

Abstract

Background & aims: Rho-kinase activation mediates cell contraction and increases intrahepatic resistance and consequently portal pressure in liver cirrhosis. Systemic Rho-kinase inhibition decreases portal pressure in cirrhosis, but also arterial pressure. Thus, liver-specific Rho-kinase inhibition is needed. The delivery of Rho-kinase inhibitor to activated hepatic stellate cells reduces fibrosis. It might also relax these contractile cells and therewith decrease intrahepatic resistance. We tested this hypothesis by performing acute experiments in cirrhotic rats.

Methods: Cirrhosis models were CCl(4)-intoxication and bile duct ligation. Three hours after injection of the Rho-kinase inhibitor (Y26732) coupled with a carrier (mannose-6-phosphate modified human serum albumin), which targets activated hepatic stellate cells, hemodynamics were analyzed by the colored microsphere technique and direct pressure measurements. The delivery site and effect of Rho-kinase inhibitor were investigated by immunohistochemical stainings, as well as Western blot. Experiments with Rho-kinase inhibitor coupled with unmodified human serum albumin served as untargeted control.

Results: In both models of cirrhosis, the carrier coupled Rho-kinase inhibitor lowered the portal pressure and decreased the hepatic-portal resistance. Immunohistochemical desmin-staining showed the carrier in hepatic stellate cells. The targeted therapy decreased the expression of the phosphorylated substrate of Rho-kinase (moesin) and abolished myosin light chains phosphorylation in fibrotic septae (collagen-staining). The targeted Rho-kinase inhibitor showed no major extrahepatic effects. By contrast, the untargeted Rho-kinase inhibitor elicited severe systemic hypotension.

Conclusions: Activated hepatic stellate cells are crucially involved in portal hypertension in cirrhosis. Targeting of Rho-kinase in hepatic stellate cells not only decreased fibrosis, as previously shown, but also lowers portal pressure acutely without major systemic effects as demonstrated in this study.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amides / pharmacology*
Animals
Hepatic Stellate Cells / drug effects*
Hepatic Stellate Cells / enzymology
Liver Cirrhosis, Experimental / drug therapy*
Liver Cirrhosis, Experimental / physiopathology
Male
Portal Pressure / drug effects*
Protein Kinase Inhibitors / pharmacology*
Pyridines / pharmacology*
Rats
Rats, Sprague-Dawley
rho-Associated Kinases / antagonists & inhibitors*
rho-Associated Kinases / metabolism

Substances

Amides
Protein Kinase Inhibitors
Pyridines
Y 27632
rho-Associated Kinases