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Vol. 283, Issue 1, 402-410, 1997
Department of Vascular and Cardiac Diseases, Parke-Davis
Pharmaceutical Research Division, Warner Lambert Company, Ann Arbor,
Michigan
The growth factors, platelet-derived growth factor (PDGF) and basic
fibroblast growth factor (bFGF) play major roles in enhanced smooth
muscle cells growth in rodent blood vessels after vascular injury.
Tyrosine kinase inhibition has been shown to be effective in blocking
tyrosine phosphorylation at the PDGF and bFGF receptors in cultured
fibroblast and vascular smooth muscle cells which in turn inhibits
their proliferation. Our study evaluated the PDGF selective tyrosine
kinase inhibitor, CGP 53716, on serum, PDGF-BB, bFGF or epidermal
growth factor-induced growth responses in cultured rat aortic smooth
muscle cells (RASMC) and Balb/3T3 fibroblasts (3T3). CGP 53716 inhibited serum-induced cell growth in RASMC, but not in 3T3 cells. CGP
53716 completely blocked PDGF-BB tyrosine receptor autophosphorylation
in RASMC and 3T3 cells, PDGF-BB-induced phosphorylation of
mitogen-activated protein kinase at 1 µM in RASMC and inhibited
PDGF-BB-induced c-Fos protein expression at 1 µM in RASMC; consistent
with inhibition of PDGF-BB-induced DNA synthesis. To examine the
selectivity of CGP 53716, PDGF-BB, bFGF or EGF-induced DNA synthesis
was measured using thymidine incorporation. CGP 53716 inhibited
PDGF-BB-, bFGF- and EGF-induced DNA synthesis in a
concentration-dependent manner in each cell line. CGP 53716 showed a 2- to 4-fold selectivity for PDGF-BB-stimulated DNA synthesis over bFGF or
EGF in RASMC or 3T3 cells. To rule out that bFGF induced the release of
endogenous PDGF, an antibody to PDGF-AB, which binds to all three
isoforms of PDGF, was coincubated with bFGF and did not suppress the
DNA synthesis induced by bFGF. Based on these results, CGP 53716 is not
selective for the PDGF receptor as previously reported. However,
EGF-stimulated receptor autophosphorylation of mitogen-activated
protein kinase phosphorylation and c-Fos protein expression were not
inhibited by CGP 53716 at 1 or 10 µM in RASMC. These findings suggest
that CGP 53716 may inhibit multiple growth factor pathways as indicated
by inhibition of DNA synthesis. However, these effects must be
downstream from the signaling for c-Fos protein expression or use an
alternate signaling route. These results further suggest that CGP 53716 may have a therapeutic potential for the treatment of vascular proliferative diseases which are stimulated by not only PDGF but other
growth factors such as bFGF and EGF.
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