Tatin which inhibits secretion of gastrin and gastric acid, hence exerts protective action on the gastric mucosa. The outcomes of the study provide harmonic coherence of gene-chip MedChemExpress FCCP analysis and biochemical assay data using samples fromCannabinoid HU210; Protective Effect on Rat StomachFigure 5. Expression of CB1 and CB2 receptors in rat pancreas and H 4065 site stomach by immunohistochemistry and western blot analyses. (A) Immunohistochemical detection of CB1 and CB2 receptors in rat pancreatic tissue sections, with the arrowheads showing the specific CB1/CB2 staining. (B) Western blot staining of CB1 and CB2 receptors in rat pancreatic tissue lysates. (C) Immunohistochemical detection of CB1 and CB2 receptors in rat stomach tissue sections, with the arrowheads showing the specific CB1/CB2 staining. (D) Western blot staining of CB1 and CB2 receptors in rat stomach tissue lysates. Note that the pancreatic acini and gastric mucosa exhibit increased immunological activity for CB1 and CB2 receptors after the induction of acute pancreatitis. (Original magnification: 6200, and scale bar = 50 mm). doi:10.1371/journal.pone.0052921.gthe animal model, suggesting a novel mechanism that the onset of AGML is, at least partly, due to the gastrin, and gastric acid /somatostain imbalance triggered by the toxins in the AP serum; and cannabinoid agonist HU210 restores the equilibrium, henceFigure 6. Effects of HU210 and AM251 on gastrin and somatostatin (SS) release from the isolated rat stomach. As described in MATERIALS AND METHODS, the levels of gastrin and somatostatin were measured in the gastric venous effluent of rats during 60 min perfusion with or without the administration of HU210 or AM251. Each specimen was measured three times and data are expressed as mean 6 SEM (n = 6). *P,0.05 vs control, #P,0.05 vs those in AP group. doi:10.1371/journal.pone.0052921.gCannabinoid HU210; Protective Effect on Rat StomachFigure 7. Effects of HU210 and AM251 on pepsin and acid output from the isolated rat stomach. The levels of pepsin and [H+] were measured in the rat gastric lumen effluent with or without the administration of HU210 or AM251. Each specimen was measured three times and data are expressed as mean 6 SEM (n = 6). *P,0.05 vs control, #P,0.05 vs those in AP group. doi:10.1371/journal.pone.0052921.gthe protection. The findings support that HU210 is beneficial for treating acute pancreatitis because of its anti-inflammation role and the preventing effect on the AGML related with acute pancreatitis. The results that the CB1 receptor antagonist AM251 fails to play any role in the AP induced gastric damage support our postulation, confirming the positive roles of CB1/2 receptors. In a prospective experiment to investigate if the proton pump inhibitors (PPIs) can protect animals with experimental acute pancreatitis, we administered omeprazole (OME, i.p., 40 mg/kg weight), a representative PPI agent, to a group of rats at the same time when AP induction was performed. The preliminary results showed that OME increased the survival rate of AP rats (data not shown). However, it may need multicenter study to elucidate if PPIs are beneficial as a therapeutic option in acute pancreatitis of humans. Taking all above, the results from our experimental investigation reveal that the inflammatory responses and the disturbances of the gastric secretion, both the endocrine and exocrine functions, are the outcomes of acute pancreatitis, and they in turn contributeto the pathogenes.Tatin which inhibits secretion of gastrin and gastric acid, hence exerts protective action on the gastric mucosa. The outcomes of the study provide harmonic coherence of gene-chip analysis and biochemical assay data using samples fromCannabinoid HU210; Protective Effect on Rat StomachFigure 5. Expression of CB1 and CB2 receptors in rat pancreas and stomach by immunohistochemistry and western blot analyses. (A) Immunohistochemical detection of CB1 and CB2 receptors in rat pancreatic tissue sections, with the arrowheads showing the specific CB1/CB2 staining. (B) Western blot staining of CB1 and CB2 receptors in rat pancreatic tissue lysates. (C) Immunohistochemical detection of CB1 and CB2 receptors in rat stomach tissue sections, with the arrowheads showing the specific CB1/CB2 staining. (D) Western blot staining of CB1 and CB2 receptors in rat stomach tissue lysates. Note that the pancreatic acini and gastric mucosa exhibit increased immunological activity for CB1 and CB2 receptors after the induction of acute pancreatitis. (Original magnification: 6200, and scale bar = 50 mm). doi:10.1371/journal.pone.0052921.gthe animal model, suggesting a novel mechanism that the onset of AGML is, at least partly, due to the gastrin, and gastric acid /somatostain imbalance triggered by the toxins in the AP serum; and cannabinoid agonist HU210 restores the equilibrium, henceFigure 6. Effects of HU210 and AM251 on gastrin and somatostatin (SS) release from the isolated rat stomach. As described in MATERIALS AND METHODS, the levels of gastrin and somatostatin were measured in the gastric venous effluent of rats during 60 min perfusion with or without the administration of HU210 or AM251. Each specimen was measured three times and data are expressed as mean 6 SEM (n = 6). *P,0.05 vs control, #P,0.05 vs those in AP group. doi:10.1371/journal.pone.0052921.gCannabinoid HU210; Protective Effect on Rat StomachFigure 7. Effects of HU210 and AM251 on pepsin and acid output from the isolated rat stomach. The levels of pepsin and [H+] were measured in the rat gastric lumen effluent with or without the administration of HU210 or AM251. Each specimen was measured three times and data are expressed as mean 6 SEM (n = 6). *P,0.05 vs control, #P,0.05 vs those in AP group. doi:10.1371/journal.pone.0052921.gthe protection. The findings support that HU210 is beneficial for treating acute pancreatitis because of its anti-inflammation role and the preventing effect on the AGML related with acute pancreatitis. The results that the CB1 receptor antagonist AM251 fails to play any role in the AP induced gastric damage support our postulation, confirming the positive roles of CB1/2 receptors. In a prospective experiment to investigate if the proton pump inhibitors (PPIs) can protect animals with experimental acute pancreatitis, we administered omeprazole (OME, i.p., 40 mg/kg weight), a representative PPI agent, to a group of rats at the same time when AP induction was performed. The preliminary results showed that OME increased the survival rate of AP rats (data not shown). However, it may need multicenter study to elucidate if PPIs are beneficial as a therapeutic option in acute pancreatitis of humans. Taking all above, the results from our experimental investigation reveal that the inflammatory responses and the disturbances of the gastric secretion, both the endocrine and exocrine functions, are the outcomes of acute pancreatitis, and they in turn contributeto the pathogenes.