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1 Department of Surgery,
The anabolic properties of insulin-like growth factor (IGF) I
are attenuated by oral diets that are low in protein. However, it is
not known whether parenteral nutrition (PN) providing a low amino acid
(AA) input will influence IGF-I action. With the use of a rat model,
this study examined the interaction between AA input (1.27 and 0.62 g
N · kg body
wt
1 · 24 h
1, AA and 1/2AA
groups, respectively) and recombinant human IGF-I (rhIGF-I, 2.5 mg · kg body
wt
1 · 24 h
1) infusion on the
composition of the carcass and organs and on plasma insulin, IGF-I,
IGF-binding protein 1 (IGFBP-1), and acid-labile subunit (ALS)
concentrations. Carcass protein deposition only occurred in the AA
groups (P < 0.003) and was not
influenced by administration of rhIGF-I. However, visceral protein loss
persisted in the AA group but was prevented by rhIGF-I infusion. The
changes in water content of the carcass and the organs were generally in the expected proportion of normal lean tissue. The accumulation of
lipid that follows the infusion of the AA-deficient PN was prevented by
rhIGF-I infusion, which may indicate an improved energy utilization.
Neither serum insulin nor ALS concentrations were influenced by the
level of AA infusion but were reduced by rhIGF-I administration.
However, plasma IGF-I levels were elevated by higher AA infusion and by
IGF-I administration. Also, IGFBP-1 concentrations were reduced by the
higher AA infusion and increased with rhIGF-I administration.
Interestingly, there was a significant interaction effect between both
of these influences. It is concluded that free IGF-I concentration,
which may be regulated by IGFBP-1 through a direct effect of AAs on the
liver, may have an important role in regulating anabolism in visceral
and possibly skeletal tissue during PN.
parenteral nutrition; insulin-like growth factor I administration; body composition; organ composition; insulin-like growth factor-binding proteins
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