IP receptor agonist-induced DNA synthesis and proliferation in primary cultures of adult rat hepatocytes: possible involvement of endogenous transforming growth factor-α

To elucidate the mechanism of action of prostaglandin I2 (PGI2) and carbaprostacyclin we studied their effect on DNA synthesis and proliferation in primary cultures of adult rat hepatocytes. Hepatocyte parenchymal cells, maintained in a serum-free, defined medium, synthesized DNA and proliferated in the presence of PGI2 (10-8 M) or carbaprostacyclin (10-9 M) in a time- and dose-dependent manner. PGI2 was less potent than carbaprostacyclin in stimulating hepatocyte mitogenesis. These effects of PGI2 and carbaprostacyclin were abolished by treatment with a specific IP receptor antagonist, CAY10441 (10-9 ~10-7 M), and by the thromboxane A2 receptor agonist, U46619 (10-7 M). Hepatocyte mitogenesis induced by the IP receptor agonists was almost completely blocked by specific inhibitors of growth-related signal transducers such as AG1478 (5 × 10-7 M), LY294002 (10-7 M), PD98059 (10-6 M), and rapamycin (10 ng/ml). In addition, PGI2 or carbaprostacyclin significantly increased the kinase activity of a (p175 kDa) receptor tyrosine kinase and the phosphorylation of p42 kDa mitogen-activated protein (MAP) kinase. Addition of a monoclonal antibody against transforming growth factor (TGF)-α, but not insulin-like growth factor-I, to the culture dose-dependently inhibited the PGI2- or carbaprostacyclin-induced hepatocyte mitogenesis. These results suggest that the IP receptor agonist-induced hepatocyte mitogenesis is mediated by autocrine secretion of TGF-α followed by activation of a receptor tyrosine kinase/MAP kinase pathway