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J. Biol. Chem., Vol. 262, Issue 11, 5408-5413, 04, 1987
I Choe, RS Aycock, R Raghow, JC Myers, JM Seyer and AH Kang
A hepatic fibrogenic factor (HFF) isolated from fibrotic rat livers has
previously been shown to stimulate the transcription of type I procollagen
genes in cultured fibroblasts (Raghow, R., Gossage, D., Seyer, J. M., and
Kang, A.H. (1984) J. Biol. Chem. 259, 12718-12723). To test if the
expression of other collagen genes was similarly affected by the fibrogenic
factor, we measured the rates of types I, III, and V procollagen synthesis
in two different cell lines after treatment with HFF. The effect of
fibrogenic factor on types I and III procollagens was tested in rat
fibroblasts, while a human rhabdomyosarcoma cell line was used to evaluate
the effect of HFF on type V procollagen synthesis. Incubation with rat
fibroblasts resulted in a 3-4-fold stimulation of the synthesis of both
types I and III procollagens in a time-dependent manner. The stimulated
rates of types I and III procollagen synthesis accompanied an increase in
the steady- state levels of their corresponding mRNAs. When A204 cells,
which are derived from a rhabdomyosarcoma and exclusively synthesize type V
procollagen, were incubated with the fibrogenic factor, a 3-4-fold
stimulation of the synthesis of both pro-alpha 1(V) and pro-alpha 2(V)
chains was seen. Using a cDNA probe for pro-alpha 2(V), we also observed
that there was a 2-3-fold increase in the steady-state level of pro-alpha
2(V) mRNA in A204 cells after treatment with the fibrogenic factor. In both
rat fibroblasts and A204 cells the steady- state levels of beta-actin mRNA
were minimally affected by fibrogenic factor, suggesting that the
procollagen genes were preferentially affected. Since types I, III, and V
collagens are present in the normal liver and accumulate aberrantly in the
fibrotic liver, we suggest that fibrogenic factor may play an important
role in determining the altered collagen composition of the fibrotic liver.
Based on these data, we also speculate that the regulation of the
biosynthesis of a variety of procollagens in diverse cell types by HFF
possibly occurs by a common mechanism.
A hepatic fibrogenic factor stimulates the synthesis of types I, III, and V procollagens in cultured cells
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