Cholecystokinin (CCK) regulates somatostatin secretion through both the CCK-A and CCK-B/gastrin receptors in sheep

Authors

  • Yana Zavros,

    1. Department of Surgery, University of Melbourne, Austin and Repatriation Medical Centre, Melbourne, Victoria 3084, Australia
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  • Arthur Shulkes

    Corresponding author
    1. Department of Surgery, University of Melbourne, Austin and Repatriation Medical Centre, Melbourne, Victoria 3084, Australia
    • To whom correspondence should be addressed.

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Abstract

  • 1Cholecystokinin (CCK) and gastrin both stimulate gastric somatostatin (SOM) secretion in vitro and thus have the potential to modulate their direct effects on the parietal cell. However, the relative potencies and the mechanisms of action of CCK and gastrin on SOM secretion in vivo have not been determined.
  • 2The objectives of the present study were to compare the in vivo potencies of the sulphated (s) and non-sulphated (ns) forms of gastrin heptadecapeptide (G-17) and CCK octapeptide (CCK-8) on SOM secretion, and to determine the nature of the receptors involved by repeating the studies in the presence of the CCK-A and CCK-B/gastrin receptor antagonists L-364,718 and L-365,260, respectively. All experiments were performed in the chronically cannulated sheep.
  • 3Dose–response experiments revealed the following potencies for SOM secretion: G-17s = CCK-8s > G-17ns ≫ CCK-8ns. However, based on the plasma levels achieved and a higher metabolic clearance rate (MCR) for CCK, CCK-8s was the most potent.
  • 4Both the CCK-A and CCK-B/gastrin receptor antagonists suppressed CCK-8s-stimulated SOM output. In contrast, G-17s-stimulated SOM output was inhibited by only the CCK-B/gastrin receptor antagonist.
  • 5Both receptor antagonists increased basal plasma gastrin and CCK levels.
  • 6The predominant circulating SOM molecular form after both gastrin and CCK stimulation was SOM-14.
  • 7In conclusion, the sulphated forms of CCK and gastrin are more potent than the non-sulphated forms. Despite sharing a common biologically active carboxy terminus, CCK stimulates SOM secretion by both the CCK-A and CCK-B/gastrin receptors, while gastrin acts via the CCK-B/gastrin receptor alone. These findings explain in part why CCK is a net inhibitor of gastric acid secretion in vivo.

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