THE C-TERMINUS OF THE PROSTAGLANDIN-E-RECEPTOR EP(3) SUBTYPE IS ESSENTIAL FOR ACTIVATION OF GTP-BINDING PROTEIN

Three isoforms of the mouse prostaglandin-E-receptor EP(3) subtype (EP(3)), EP(3 alpha) EP(3 beta) and EP(3 gamma) with different C-termini, which are produced through alternative splicing, showed different efficiencies with respect to heterotrimeric GTP-binding protein activation and adenylate cyclase inhibition [Sugimoto, Y., Negishi, M., Hayashi, Y., Namba, T., Honda, A., Watabe, A., Hirata, M., Narumiya, S. & Ichikawa, A, (1993) J. Biol. Chem. 268, 2712-2718; Irie, A., Sugimoto, Y., Namba, T., Harazono, A., Honda, A., Watabe, A., Negishi, M., Narumiya, S. & Ichikawa, A. (1993) Eur: J. Biochem. 217, 313-318]. To assess the role of the C-terminus in GTP-binding protein coupling, we truncated the C-terminus of EP(3) at an alternative splicing site and expressed the mutant receptor. The truncated receptor retained the ability to physically associate with G(i2) forming an agonist/ receptor/G(i2), ternary complex, and to undergo the characteristic conversion of its agonist-binding affinity, mediated by a guanine nucleotide from a low-affinity state to a high-affinity state. However, sulprostone, an EP(3) agonist, failed not only to inhibit the forskolin-induced cAMP accumulation in the mutant receptor-expressing cells but also to stimulate the GTPase activity in the mutant receptor-expressing cell membrane. These results indicated that the C-terminus of EP(3) is essential for the activation of GTP-binding protein.