The molecular mechanism of gypenosides-induced G1 growth arrest of rat hepatic stellate cells

Abstract Aim of the study Gypenosides, the saponins extract derived from Gynostemma pentaphyllum Makino, have been used for treating hepatitis and cancer in Asia. Our previous study demonstrates that gypenosides inhibit the onset and improve the recovery of liver fibrosis induced by CCl 4 in rats. In this study, we used the isolated rat hepatic stellate cells (HSCs) as a model to study the cellular mechanism of gypenosides-inhibited liver fibrosis. Materials and methods Rat HSCs was treated with PDGF, gypenosides or vehicle. Cell viability was assessed by trypan blue staining. Apoptosis and cell cycle were evaluated by flow cytometry. The activation or inhibition of signal molecules was detected by Western blotting. Results Our results showed that 500 μg/ml gypenosides decreased PDGF-induced rat HSCs numbers (8750 ± 2629 versus 103,000 ± 6683, p 1 phase without the presence of sub-G 1 fraction. Analysis of PDGF-induced proliferative molecules including phosphorylation of Akt and p70 S6K , gypenosides inhibited the activation of this signal pathway. Furthermore, gypenosides down-regulated the protein expression of cell cycle G 1 -specific cyclin D1 and D3. Conclusions Gypenosides inhibited PDGF-induced HSCs proliferation by inhibiting the signal pathway of PDGF-Akt-p70 S6K and down-regulation of cyclin D1 and D3 expression.