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Diabetes, Vol 24, Issue 12 1050-1056, Copyright © 1975 by American Diabetes Association
Gastric inhibitory polypeptide. Its physiologic release and insulinotropic action in the dog
RA Pederson, HE Schubert and JC Brown
Studies were carried out in conscious dogs in which the immunoreactive
gastric inhibitory polypeptide (IR-GIP) response to graded doses of oral
fat (triglycerides) and glucose was investigated. The IR-GIP response to
the doses of triglycerides used was greater and more prolonged than the
response to the glucose loads employed. In addition, the relative
insulinotropic potencies of exogenous porcine GIP and IR-GIP released by
fat as against those released by oral glucose were assessed. When glucose
was administered by the oral route, the immunoreactive insulin (IRI)
response was magnified above the IRI response to a comparable intravenous
glucose load. The serum IRI response to oral glucose was accompanied by a
concomitant rise in serum IR-GIP levels, suggesting a causal relationship.
IR-GIP released by oral fat was shown to augment the IRI response to an
intravenous glucose load, resulting in an improvement of glucose tolerance.
Fat-released IR-GIP augmented IRI levels to a lessor degree than either
oral glucose or an infusion of porcine GIP.

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Copyright © 1975 by the American Diabetes Association.
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