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Vol. 281, Issue 1, 522-530, 1997
Department of Pharmacology, Cephalon, Inc., West Chester,
Pennsylvania
Recent studies indicate that a daily s.c. injection of 1 mg/kg of
recombinant human insulin-like growth factor-1 (rhIGF-1) for 17 days is
efficacious in enhancing the functional recovery of injured sciatic
nerves in CD-1 mice. To identify and characterize surrogate marker(s)
that are altered in association with the administration of an
efficacious dose of rhIGF-1, dose-response curves (0.1, 1 and 10 mg/kg)
and time course effects (0, 0.5, 3, 6 and 24 hr) were determined after
acute (single) and chronic (once daily for 17 days) injections of
rhIGF-1 in CD-1 mice. Plasma glucose levels decreased in a
dose-dependent fashion after either acute or chronic injections of
rhIGF-1 with maximal effects at 0.5 to 1 hr after administration of
rhIGF-1. Among the three insulin-like growth factor binding proteins
(IGFBPs) evaluated in the study, only IGFBP2 levels were consistently
increased in a dose-dependent fashion with maximal effects 3 hr after
the last of a series of injections of rhIGF-1. Furthermore, IGFBP2
levels increased at a dose of rhIGF-1 (1 mg/kg) that enhances the
regeneration of injured sciatic nerves in mice. Chronic administration
of insulin at doses that cause comparable decreases in plasma glucose
to that of rhIGF-1 did not alter IGFBP2 levels or enhance hindlimb function suggesting that the beneficial effects of rhIGF-1 occur via
activation of the type-I IGF receptor rather than the insulin receptor.
Based on these criteria, IGFBP2 appears to be useful as a surrogate
marker for determining the in vivo effects of rhIGF-1.
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