Physiological hypoxia prevents bile salt-induced apoptosis in human and rat hepatocytes

Simon Hohenester; Timo Vennegeerts; Michaela Wagner; Ralf Wimmer; Heidrun Drolle; Christina Rieger; Gerald U Denk; Christian Rust; Michael Fiegl

doi:10.1111/liv.12368

Physiological hypoxia prevents bile salt-induced apoptosis in human and rat hepatocytes

Liver Int. 2014 Sep;34(8):1224-31. doi: 10.1111/liv.12368. Epub 2013 Nov 20.

Authors

Simon Hohenester¹, Timo Vennegeerts, Michaela Wagner, Ralf Wimmer, Heidrun Drolle, Christina Rieger, Gerald U Denk, Christian Rust, Michael Fiegl

Affiliation

¹ Department of Medicine II, University of Munich, Munich, Germany.

PMID: 24164780
DOI: 10.1111/liv.12368

Abstract

Background & aims: Hydrophobic bile salts such as glycochenodeoxycholate (GCDC) accumulate in cholestatic liver disease and induce hepatocellular apoptosis, promoting profibrotic signalling. The tissue microenvironment is an integral player in cellular pathophysiology, but it is not routinely incorporated into laboratory studies. Tissue oxygen partial pressure (pO₂) may be an underestimated component of the microenvironment: in the liver, a pO₂ of 30-45 mmHg (approximately 6% O₂) is physiological, because of predominant portal blood supply. It was the aim of this project to investigate the impact of physiological hypoxia (i.e. 6% O₂) on hepatocellular function, namely, bile salt-induced apoptosis.

Methods: Human hepatoma cells (HepG2-Ntcp) and primary rat hepatocytes were cultured at standard laboratory (hyperoxic) conditions (21% O₂) and at physiological hypoxia (6% O₂) in parallel for 1-8 days to study hepatocellular apoptosis and activation of signalling pathways. Standard laboratory analyses were applied for bile salt uptake, caspase-3/-7 activity, western blotting and gene-array analysis.

Results: Culturing at physiological hypoxia protected both human and rat hepatocytes against GCDC-induced apoptosis: caspase-3/-7 activation was diminished by 3.1 ± 0.5-fold in human HepG2-Ntcp and completely abolished in primary rat hepatocytes. Bile salt uptake was unaffected. Induction of hypoxia-inducible factor-1α indicated adaption to physiological hypoxia. The MEK/ERK cascade was activated and anti-apoptotic mediators were induced: N-Myc down-regulated gene, gelsolin and carbonic anhydrase IX were upregulated 12.4-, 6.5- and 5.2-fold respectively.

Conclusions: We conclude from these data that (i) physiological hypoxia protects hepatocytes from bile salt-induced apoptosis, (ii) tissue pO₂ is a crucial, underestimated component of the microenvironment and should (iii) be considered when studying hepatocellular physiology in vitro.

Keywords: apoptosis; bile salt; liver; physiological hypoxia.

Publication types

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

MeSH terms

Animals
Apoptosis / drug effects
Apoptosis / physiology*
Bile Acids and Salts / adverse effects
Blotting, Western
Cell Cycle Checkpoints / drug effects
Cell Cycle Checkpoints / physiology*
Cell Hypoxia / physiology*
Flow Cytometry
Hep G2 Cells
Hepatocytes / physiology*
Humans
Hypoxia-Inducible Factor 1, alpha Subunit / metabolism*
Microarray Analysis
Rats
Signal Transduction / physiology

Substances

Bile Acids and Salts
Hypoxia-Inducible Factor 1, alpha Subunit