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Diabetes, Vol 47, Issue 12 1824-1835, Copyright © 1998 by American Diabetes Association
Differential regulation of amino acid exchange and protein dynamics across splanchnic and skeletal muscle beds by insulin in healthy human subjects
SE Meek, M Persson, GC Ford and KS Nair
Division of Endocrinology, Mayo Clinic and Foundation, Rochester, Minnesota 55905, USA.
To define the mechanism of insulin's anticatabolic action, the effects of
three different dosages of insulin (0.25, 0.5, and 1.0 mU x kg(-1) x
min(-1)) versus saline on protein dynamics across splanchnic and skeletal
muscle (leg) beds were determined using stable isotopes of phenylalanine,
tyrosine, and leucine in 24 healthy subjects. After an overnight fast,
protein breakdown in muscle exceeded protein synthesis, causing a net
release of amino acids from muscle bed, while in the splanchnic bed protein
synthesis exceeded protein breakdown, resulting in a net uptake of these
amino acids. Insulin decreased (P < 0.003) muscle protein breakdown in a
dose-dependent manner with no effect on muscle protein synthesis, thus
decreasing the net amino acid release from the muscle bed. In contrast,
insulin decreased protein synthesis (P < 0.03) in the splanchnic region
with no effect on protein breakdown, thereby decreasing the net uptake of
the amino acids. In addition, insulin also decreased (P < 0.001) leucine
nitrogen flux substantially more than leucine carbon flux, indicating
increased leucine transamination (an important biochemical process for
nitrogen transfer between amino acids and across the organs), in a
dose-dependent manner, with the magnitude of effect being greater on
skeletal muscle than on the splanchnic bed. In conclusion, muscle is in a
catabolic state in human subjects after an overnight fast and provides
amino acids for synthesis of essential proteins in the splanchnic bed.
Insulin achieves amino acid balance across splanchnic and skeletal muscle
beds through its differential effects on protein dynamics in these tissue
beds.

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Copyright © 1998 by the American Diabetes Association.
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