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Department of Medicine, University of North Carolina School of Medicine, Chapel Hill, North Carolina 27599
Address all correspondence and requests for reprints to: David R. Clemmons, M.D., Department of Medicine, CB 7170, University of North Carolina School of Medicine, Chapel Hill, North Carolina 27599-7170.
Insulin-like growth factor (IGF)-binding protein-5 (IGFBP-5) is cleaved
by a serine protease that is secreted by fibroblasts and porcine smooth
muscle cells (pSMC) in culture. To investigate whether other serine
proteases could cleave this substrate at physiologically relevant
concentrations, we determined the proteolytic effects of thrombin on
IGFBP-5. Human 
-thrombin (0.0008 NIH U/ml) cleaved IGFBP-5 into
24-, 23-, and 20-kDa non-IGF-I-binding fragments. Cleavage occurred at
a physiologically relevant thrombin concentration. The effect was
specific for IGFBP-5, as other forms of IGFBPs, e.g.
IGFBP-1, IGFBP-2, and IGFBP-4 were not cleaved by thrombin. Although
IGFBP-3 was cleaved by thrombin, this effect required a 50-fold greater
thrombin concentration. [35S]Methionine labeling followed
by immunoprecipitation confirmed that IGFBP-5 that was constitutively
synthesized by pSMC cultures was also degraded by thrombin into 24-,
23-, and 20-kDa fragments. The binding of IGF-I to IGFBP-5 partially
inhibited IGFBP-5 degradation by thrombin, and an IGF analog that does
not bind to IGFBP-5 had no effect. Thrombin did not account for the
serine protease activity that had been shown previously to be present
in pSMC-conditioned medium. This was proven by showing that 1) no
immunoreactive thrombin could be detected in the pSMC-conditioned
medium; 2) the IGFBP-5 fragments that were generated by thrombin showed
three cleavage sites (Arg192-Ala193,
Arg156-Ile157, and
Lys120-His121), whereas the serine protease in
conditioned medium cleaves IGFBP-5 at a different site; and 3) hirudin
had no effect on IGFBP-5 cleavage by the protease in pSMC medium;
however, it inhibited IGFBP-5 degradation by thrombin. To determine the
physiological significance of IGFBP-5 cleavage, the effect of an
IGFBP-5 mutant that is resistant to cleavage by the pSMC protease and
has been shown to inhibit IGF-I actions in pSMC was determined. This
mutant inhibited IGF-I-stimulated DNA synthesis, but if thrombin was
added simultaneously, IGF-I was fully active. In summary, physiological
concentrations of thrombin degrade IGFBP-5. Degradation can be blocked
by hirudin and is partially inhibited by IGF-I binding. Generation of
active thrombin in vessel walls may be a physiologically relevant
mechanism for controlling IGF-I bioactivity.
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