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Diabetes, Vol 45, Issue 5 552-556, Copyright © 1996 by American Diabetes Association
The effect of glucagon-like peptide I (GLP-I) on glucose elimination in healthy subjects depends on the pancreatic glucoregulatory hormones
M Toft-Nielson, S Madsbad and JJ Holst
Department of Endocrinology, Hvidovre Hospital, Copenhagen, Denmark.
Glucagon-like peptide I (GLP-I) decreases plasma glucose in type II
diabetic patients and in healthy subjects indirectly by stimulation of
insulin and inhibition of glucagon secretion, whereby the hepatic glucose
production decreases. However, recent studies indicate that GLP-I may also
directly influence peripheral and hepatic glucose uptake. We infused
somatostatin (SS) intravenously (500 or 1,000 microgram/h) in 13 healthy
subjects to suppress insulin and glucagon secretion from the endocrine
pancreas, together with infusion of either GLP-I (50 pmol / kg / h) or
saline intravenously. After 30 min, a 25-g intravenous glucose tolerance
test (IVGTT) was carried out, and plasma concentrations of glucose,
insulin, glucagon, and GLP-I were measured during the following 2 h. IVGTT
together with GLP-I infusion significantly elevated insulin during 500
microgram/h SS but not during 1,000 microgram/h SS. Plasma glucagon was
strongly depressed in all experiments. During 500 microgram/h SS, the
glucose disappearance constant, Kg, was 0.49 +/- 0.03% per minute with
GLP-I and 0.39 +/- 0.04% per minute with saline (n = 8, P = 0.004). With
1,000 microgram/h SS, Kg was 0.42 +/- 0.03% per minute with GLP-I and 0.40
+/- 0.03% per minute without (NS). In conclusion, when endogenous insulin
secretion is held at a constant low level, which may be accomplished only
with very large doses of SS, GLP-I has no effect on glucose elimination.
Thus, an insulin-independent effect of GLP-I on glucose disposal could not
be demonstrated.

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Copyright © 1996 by the American Diabetes Association.
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