Angiotensin II protects primary rat hepatocytes against bile salt-induced apoptosis

PLoS One. 2012;7(12):e52647. doi: 10.1371/journal.pone.0052647. Epub 2012 Dec 26.

Abstract

Angiotensin II (AT-II) is a pro-fibrotic compound that acts via membrane-bound receptors (AT-1R/AT-2R) and thereby activates hepatic stellate cells (HSCs). AT-II receptor blockers (ARBs) are thus important candidates in the treatment of liver fibrosis. However, multiple case reports suggest that AT-1R blockers may induce hepatocyte injury. Therefore, we investigated the effect of AT-II and its receptor blockers on cytokine-, oxidative stress- and bile salt-induced cell death in hepatocytes. Primary rat hepatocytes were exposed to TNF-α/Actinomycin D, the ROS-generating agent menadione or the bile salts: glycochenodeoxycholic acid (GCDCA) and tauro-lithocholic acid-3 sulfate (TLCS), to induce apoptosis. AT-II (100 nmol/L) was added 10 minutes prior to the cell death-inducing agent. AT-1R antagonists (Sartans) and the AT-2R antagonist PD123319 were used at 1 µmol/L. Apoptosis (caspase-3 activity, acridine orange staining) and necrosis (Sytox green staining) were quantified. Expression of CHOP (marker for ER stress) and AT-II receptor mRNAs were quantified by Q-PCR. AT-II dose-dependently reduced GCDCA-induced apoptosis of hepatocytes (-50%, p<0.05) without inducing necrosis. In addition, AT-II reduced TLCS-induced apoptosis of hepatocytes (-50%, p<0.05). However, AT-II did not suppress TNF/Act-D and menadione-induced apoptosis. Only the AT-1R antagonists abolished the protective effect of AT-II against GCDCA-induced apoptosis. AT-II increased phosphorylation of ERK and a significant reversal of the protective effect of AT-II was observed when signaling kinases, including ERK, were inhibited. Moreover, AT-II prevented the GCDCA-induced expression of CHOP (the marker of the ER-mediated apoptosis).

Conclusion: Angiotensin II protects hepatocytes from bile salt-induced apoptosis through a combined activation of PI3-kinase, MAPKs, PKC pathways and inhibition of bile salt-induced ER stress. Our results suggest a mechanism for the observed hepatocyte-toxicity of Sartans (angiotensin receptor blockers, ARBs) in some patients with chronic liver injury.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Angiotensin II / pharmacology
  • Angiotensin II / physiology*
  • Animals
  • Apoptosis*
  • Caspase 3 / metabolism
  • Cell Shape / drug effects
  • Cells, Cultured
  • Dactinomycin / pharmacology
  • Endoplasmic Reticulum Stress
  • Enzyme Activation
  • Glycochenodeoxycholic Acid / pharmacology*
  • Glycochenodeoxycholic Acid / physiology
  • Hepatocytes / drug effects
  • Hepatocytes / physiology*
  • MAP Kinase Signaling System
  • Male
  • Oxidative Stress
  • Phosphatidylinositol 3-Kinases / metabolism
  • Primary Cell Culture
  • Protein Kinase C / metabolism
  • Rats
  • Rats, Wistar
  • Reactive Oxygen Species / metabolism
  • Receptor, Angiotensin, Type 1 / metabolism
  • Taurolithocholic Acid / analogs & derivatives*
  • Taurolithocholic Acid / pharmacology
  • Taurolithocholic Acid / physiology
  • Tumor Necrosis Factor-alpha / pharmacology
  • Tumor Necrosis Factor-alpha / physiology
  • Vitamin K 3 / pharmacology

Substances

  • Reactive Oxygen Species
  • Receptor, Angiotensin, Type 1
  • Tumor Necrosis Factor-alpha
  • Angiotensin II
  • taurolithocholic acid 3-sulfate
  • Dactinomycin
  • Taurolithocholic Acid
  • Glycochenodeoxycholic Acid
  • Vitamin K 3
  • Phosphatidylinositol 3-Kinases
  • Protein Kinase C
  • Casp3 protein, rat
  • Caspase 3

Grants and funding

This research was funded by the University of Groningen. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.