Abstract

We have investigated the actions of 17β-estradiol (E2) on the production of cAMP stimulated by synthetic human PTH [hPTH-(l–34)], synthetic hPTH-related protein [hPTHrP-(l–34)]( and vasoactive intestinal peptide (VIP) in human (SaOS-2) and rat (ROS 17/2.8) osteoblast-like osteosarcoma cells. In SaOS-2 cells, hPTH-(l–34) (2.5 nM), hPTHrP- (1–34) (2.5 nM), and VIP (10–100 nM) stimulated the accumulation of cAMP markedly (>20- to 30-fold in 1 h). Cells were preincubated in serum-free medium for 4–24 h, then in the absence or presence of E2 for 4 h before a 1-h stimulation with peptide hormone in the absence of E2. In SaOS-2 cells, pretreatment with E2 (10-12-10-8 M) for 4 h inhibited by up to 50% the accumulation of cAMP stimulated by hPTH-(l–34) or hPTHrP- (1–34), but E2 had no inhibitory effect on VIP action. 17α- Estradiol had no inhibitory action on hPTH- or hPTHrPstimulated accumulation of cAMP at concentrations as high as 10-8 M. Additional evidence against a nonspecific effect of E2 was the total lack of inhibition of cAMP accumulation stimulated by hPTH-(l–34) or hPTHrP-(l–34) in ROS 17/2.8 cells at concentrations of E2 up to 10-6 M. We conclude that E2 can act directly and rapidly in human osteoblast-like cells to modulate selectively the ability of hPTH and hPTHrP to enhance the production of cAMP. (Endocrinology124: 397–401, 1989)