Gastroenterology
Volume 138, Issue 2 , Pages 715-725, February 2010

Biliary Acute Pancreatitis in Mice is Mediated by the G-Protein−Coupled Cell Surface Bile Acid Receptor Gpbar1

  • George Perides

      Affiliations

    • Department of Surgery, Tufts Medical Center and Tufts University School of Medicine, Boston, Massachusetts
    • Corresponding Author InformationReprint requests Address requests for reprints to: George Perides, PhD, Department of Surgery, Tufts Medical Center, 750 Washington Street, Boston, Massachusetts 02111. fax: (617) 636-1466
    • ,
  • Johanna M. Laukkarinen

      Affiliations

    • Department of Gastroenterology and Alimentary Tract Surgery, Tampere University Hospital, Tampere, Finland
    • ,
  • Galya Vassileva

      Affiliations

    • Department of Discovery Technologies, Schering–Plough Research Institute, Kenilworth, New Jersey
    • ,
  • Michael L. Steer

      Affiliations

    • Department of Surgery, Tufts Medical Center and Tufts University School of Medicine, Boston, Massachusetts

Received 18 May 2009; accepted 23 October 2009. published online 09 November 2009.

Background & Aims

The mechanisms by which reflux of bile acids into the pancreas induces pancreatitis are unknown. We reasoned that key events responsible for this phenomenon might be mediated by Gpbar1, a recently identified and widely expressed G-protein−coupled, cell surface bile acid receptor.

Methods

Acute pancreatitis was induced in wild-type and Gpbar1−/− mice by either retrograde ductal infusion of taurolithocholic acid-3-sulfate (TLCS) or supramaximal secretagogue stimulation with caerulein. In vitro experiments were performed in which acini obtained from wild-type and Gpbar1−/− mice were exposed to either submicellar concentrations of TLCS (200−500 μM) or a supramaximally stimulating concentration of caerulein (10 nM).

Results

Gpbar1 is expressed at the apical pole of acinar cells and its genetic deletion is associated with reduced hyperamylasemia, edema, inflammation, and acinar cell injury in TLCS-induced, but not caerulein-induced, pancreatitis. In vitro, genetic deletion of Gpbar1 is associated with markedly reduced generation of pathological calcium transients, intracellular activation of digestive zymogens, and cell injury when these responses are induced by exposure to TLCS, but not when they are induced by exposure to caerulein.

Conclusions

Gpbar1 may play a critical role in the evolution of bile-acid−induced pancreatitis by coupling exposure to bile acids with generation of pathological intracellular calcium transients, intra-acinar cell zymogen activation, and acinar cell injury. Acute biliary pancreatitis may be a “receptor-mediated” disease and interventions that interfere with Gpbar1 function might prove beneficial in the treatment and/or prevention of biliary acute pancreatitis.

Abbreviations used in this paper: BAPTA, 1,2-bis(2-aminophenoxy)ethane-N,N,N,N′-tetraacetic acid, Gpbar1, G-protein−coupled bile acid receptor-1, LDH, lactate dehydrogenase, TLCS, taurolithocholic acid 3-sulfate sodium salt

 

 Conflicts of interest The authors disclose no conflicts.

 Funding Supported by National Institutes of Health grant RO-1 31396 from National Institute of Diabetes, Digestive and Kidney Diseases (M.L.S.), P30-NS047423 and by a fellowship from Sigrid Jusélius Foundation, Finland (J.M.L.).

PII: S0016-5085(09)01949-0

doi:10.1053/j.gastro.2009.10.052

Refers to article:

  • The Role of Bile Acids in Gallstone-Induced Pancreatitis , 23 December 2009

    Markus M. Lerch, Ali A. Aghdassi
    Gastroenterology February 2010 (Vol. 138, Issue 2, Pages 429-433)

Gastroenterology
Volume 138, Issue 2 , Pages 715-725, February 2010