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Vol. 283, Issue 2, 611-618, 1997
Department of Pharmaceutics, Faculty of Pharmaceutical Sciences,
Okayama University, Okayama, Japan
The GI absorption of recombinant human insulin-like growth factor-I
(rhIGF-I) and its improvement were investigated in rats. The
125I-rhIGF-I rapidly degraded to the trichloroacetic
acid-soluble form in the small-intestinal contents, but it was
relatively stable in the gastric and large-intestinal contents and in
the subcellular fraction of the small-intestinal mucosa. To protect
rhIGF-I from degradation in the small-intestinal contents, the effect
of some adjuvants was examined and their degradation was markedly
inhibited by the presence of aprotinin or casein. After p.o.
administration of 125I-rhIGF-I at the dose of 1.0 mg/kg,
trichloroacetic acid-precipitable radioactivity in the plasma was
periodically determined. We found that a considerable amount of rhIGF-I
was absorbed into the systemic circulation and that the bioavailability
was 9.3%, which is much greater than that of insulin. The
coadministration of aprotinin and that of casein enhanced the
bioavailability further: 46.9% and 67.0%, respectively.
Radioimmunoassay using a monoclonal antibody for rhIGF-I confirmed the
high bioavailability of immunoreactive rhIGF-I. From gel chromatography
of plasma, the radioactivity in the plasma was found to be in the form
of high-molecular-weight complexes. The mechanism for the uptake of
rhIGF-I by intestinal mucosa may be absorptive-mediated endocytosis.
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