Vol. 276, Issue 4, E806-E813, April 1999
Effect of a selective rise in hepatic artery insulin on
hepatic glucose production in the conscious dog
Dana K.
Sindelar,
Kayano
Igawa,
Chang A.
Chu,
Jim H.
Balcom,
Doss W.
Neal, and
Alan D.
Cherrington
Department of Molecular Physiology and Biophysics, Vanderbilt
University School of Medicine, Nashville, Tennessee 37232-0615
In the present study we compared the hepatic
effects of a selective increase in hepatic sinusoidal insulin brought
about by insulin infusion into the hepatic artery with those resulting from insulin infusion into the portal vein. A pancreatic clamp was used
to control the endocrine pancreas in conscious overnight-fasted dogs.
In the control period, insulin was infused via peripheral vein and the
portal vein. After the 40-min basal period, there was a 180-min test
period during which the peripheral insulin infusion was stopped and an
additional 1.2 pmol · kg
1 · min1
of insulin was infused into the hepatic artery (HART,
n = 5) or the portal vein (PORT,
n = 5, data published previously). In the HART
group, the calculated hepatic sinusoidal insulin level increased from
99 ± 20 (basal) to 165 ± 21 pmol/l (last 30 min). The
calculated hepatic artery insulin concentration rose from 50 ± 8 (basal) to 289 ± 19 pmol/l (last 30 min). However, the overall arterial (50 ± 8 pmol/l) and portal vein insulin levels (118 ± 24 pmol/l) did not change over the course of the experiment. In the PORT group, the calculated hepatic sinusoidal insulin level increased from 94 ± 30 (basal) to 156 ± 33 pmol/l
(last 30 min). The portal insulin rose from 108 ± 42 (basal) to 192 ± 42 pmol/l (last 30 min), whereas the overall arterial insulin (54 ± 6 pmol/l) was unaltered during the study. In both groups hepatic
sinusoidal glucagon levels remained unchanged, and euglycemia was
maintained by peripheral glucose infusion. In the HART group, net
hepatic glucose output (NHGO) was suppressed from 9.6 ± 2.1 µmol · kg1 · min1 (basal) to 4.6 ± 1.0 µmol · kg1 · min1
(15 min) and eventually fell to 3.5 ± 0.8 µmol · kg1 · min1
(last 30 min, P < 0.05). In the PORT
group, NHGO dropped quickly (P < 0.05) from 10.0 ± 0.9 (basal) to 7.8 ± 1.6 (15 min) and eventually reached 3.1 ± 1.1 µmol · kg1 · min1
(last 30 min). Thus NHGO decreases in response to a selective increase
in hepatic sinusoidal insulin, regardless of whether it comes about
because of hyperinsulinemia in the hepatic artery or portal vein.
glycogenolysis; gluconeogenesis
