PLoS ONE (Feb 2008)

Cannabinoids reduce markers of inflammation and fibrosis in pancreatic stellate cells.

  • Christoph W Michalski,
  • Milena Maier,
  • Mert Erkan,
  • Danguole Sauliunaite,
  • Frank Bergmann,
  • Pal Pacher,
  • Sandor Batkai,
  • Nathalia A Giese,
  • Thomas Giese,
  • Helmut Friess,
  • Jörg Kleeff

DOI
https://doi.org/10.1371/journal.pone.0001701
Journal volume & issue
Vol. 3, no. 2
p. e1701

Abstract

Read online

BackgroundWhile cannabinoids have been shown to ameliorate liver fibrosis, their effects in chronic pancreatitis and on pancreatic stellate cells (PSC) are unknown.Methodology/principal findingsThe activity of the endocannabinoid system was evaluated in human chronic pancreatitis (CP) tissues. In vitro, effects of blockade and activation of cannabinoid receptors on pancreatic stellate cells were characterized. In CP, cannabinoid receptors were detected predominantly in areas with inflammatory changes, stellate cells and nerves. Levels of endocannabinoids were decreased compared with normal pancreas. Cannabinoid-receptor-1 antagonism effectuated a small PSC phenotype and a trend toward increased invasiveness. Activation of cannabinoid receptors, however, induced de-activation of PSC and dose-dependently inhibited growth and decreased IL-6 and MCP-1 secretion as well as fibronectin, collagen1 and alphaSMA levels. De-activation of PSC was partially reversible using a combination of cannabinoid-receptor-1 and -2 antagonists. Concomitantly, cannabinoid receptor activation specifically decreased invasiveness of PSC, MMP-2 secretion and led to changes in PSC phenotype accompanied by a reduction of intracellular stress fibres.Conclusions/significanceAugmentation of the endocannabinoid system via exogenously administered cannabinoid receptor agonists specifically induces a functionally and metabolically quiescent pancreatic stellate cell phenotype and may thus constitute an option to treat inflammation and fibrosis in chronic pancreatitis.