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Diabetes, Vol 43, Issue 2 232-239, Copyright © 1994 by American Diabetes Association
Regulation of insulin-like growth factor-binding protein-1 in rat serum
MS Lewitt, H Saunders, JL Phyual and RC Baxter
Department of Endocrinology, Royal Prince Alfred Hospital, Sydney, Australia.
Previous studies support a role for insulin-like growth factor-binding
protein-1 (IGFBP-1) in modulating insulin-like growth factor (IGF)
availability for glucose homeostasis. We have developed a radioimmunoassay
(RIA) for rat IGFBP-1 (rIGFBP-1) and have examined the regulation of
circulating levels by nutritional and hormonal status. Rabbit antisera were
raised against pure rIGFBP-1, and an assay was established with a
sensitivity of 50 pg. In the rat, serum IGFBP-1 concentrations decrease
with increasing developmental age. They were highest in fetal rat serum,
exceeding 4 mg/L, and decreased to < 0.1 mg/L in adult animals. Serum
rIGFBP-1 levels increased during fasting, 6-fold after 24 h and 18-fold
after 48 h, and were suppressed to levels identical to ad libitum-fed
control rats within 2 h of refeeding. Fasting levels were > 2-fold
higher in female than male animals. IGFBP-1 concentrations were suppressed
by > 50% in two rat models of insulin resistance. Levels increased in
STZ-induced (streptozotocin) diabetes and were suppressed to normal with
insulin treatment. Exercise stimulated rIGFBP-1 concentrations in fasting
animals. On immunoblotting after SDS-PAGE (sodium dodecyl
sulfate-polyacrylamide gel electrophoresis), rIGFBP-1 in serum appeared as
a doublet with molecular masses at 31 and 33 kD. The components of this
doublet did not vary across the range of experimental conditions. These
observations indicate that the pattern of regulation of rIGFBP-1 is similar
to that seen in previous studies of human IGFBP-1, with age, sex, and
nutritional status being important regulators.(ABSTRACT TRUNCATED AT 250
WORDS)

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Copyright © 1994 by the American Diabetes Association.
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