Changes in collagen metabolism in response to endothelin-1: Evidence for fibroblast heterogeneity

Eudothelin-1 (Et-1) is a 21-amino acid peptide primarily synthesized by endothelial cells. It was originally classified as a potent vasoconstrictor but recent evidence suggests that it also possesses a wide variety of non-vascular actions. It stimulates fibroblast and smooth muscle cell proliferation and it has been shown to stimulate fibroblast collagen metabolism. However, studies on its ability to regulate collagen production remain incomplete, and its effect on post-tranclational processing of procollagen has not been studied. This report details the effect of Et-1 on the rates of procollagen synthesis and degradation in two fibroblast cell lines; human foetal lung (HFL-1) and whole foetal rat fibroblasts (Rat 2). Fibroblast cultures were incubated for 24 hr in the presence or absence of Et-1 before procollagen metabolism was determined by measuring hydroxyproline. Non-collagen metabolism was also determined in these cultures from the uptake of tritiated pbenylalanine. Et-1 stimulated procollagen synthesis in HFL-1 fibroblasts and reduced synthesis in Rat 2 cells. The response was dose dependent with the greatest effect at 1.10 −6M Et-1 for both cell types (155 ± 6% of control (mean ± SD, n = 6, P < 0.01) and 61 ± 4% of control ( n = 4, P < 0.01) for IHFIA and Rat 2 fibroblasts, respectively). Non-collagen protein synthesis was increased to 148 ± 5% of control ( P < 0.05) at 1.10 −6 M Et-1. Non-collagen protein synthesis remained unaffected in the HFL-1 fibroblast cultures. Procollagen degradation, expressed as a proportion of total procollagen synthesis, was decreased in HFL-1 fibroblasts (control, 29 ± 2%; Et-1, 1.10 −6 M; 21 ± 2%; P < 0.01), and increased in Rat 2 fibroblasts (control 42 ± 1%; Et-1, 1.10 −6 M; 49 ± 1%; P < 0.01). Blocking of the Et A receptor for Et-1, using the receptor antagonist- BQ123, abolished the effect of Et-1 on procollsgen metabolism in both cell types. These results suggest that different populations of fibroblasts exhibit heterogeneous responses to Et-1. It is concluded that Et-1 may play an important role in the extent and distribution of fibrosis seen in diseases associated with the overproduction of Et-1.