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Two Possibly Distinct Prostaglandin E1 Receptors in N1E-115 Clone: One Mediating Inositol Trisphosphate Formation, Cyclic GMP Formation, and Intracellular Calcium Mobilization and the Other Mediating Cyclic AMP Formation
Authors:Shigenobu Kanba  Nobuyuki Sasakawa  Toshio Nakaki  Kiyoko-Shimizu Kanba  Gohei Yagi  Ryuichi Kato  Elliott Richelson
Institution:Department of Neuro-psychiatry, Keio University School of Medicine, Tokyo, Japan.
Abstract:Prostaglandin E1 (PGE1)-mediated transmembrane signal control systems were investigated in intact murine neuroblastoma cells (clone N1E-115). PGE1 increased intracellular levels of total inositol phosphates (IP), cyclic GMP, cyclic AMP, and calcium (Ca2+]i). PGE1 transiently increased inositol 1,4,5-trisphosphate formation, peaking at 20 s. There was more than a 10-fold difference between the ED50 for PGE1 at cyclic AMP formation (70 nM) and its ED50 values at IP accumulation (1 microM), cyclic GMP formation (2 microM), and Ca2+]i increase (5 microM). PGE1-mediated IP accumulation, cyclic GMP formation, and Ca2+]i increase depended on both the concentration of PGE1 and extracellular calcium ions. PGE1 had more potent intrinsic activity in cyclic AMP formation, IP accumulation, and cyclic GMP formation than did PGE2, PGF2 alpha, or PGD2. A protein kinase C activator, 4 beta-phorbol 12 beta-myristate 13 alpha-acetate, had opposite effects on PGE1-mediated IP release and cyclic GMP formation (inhibitory) and cyclic AMP formation (stimulatory). These data suggest that there may be subtypes of the PGE1 receptor in this clone: a high-affinity receptor mediating cyclic AMP formation, and a low-affinity receptor mediating IP accumulation, cyclic GMP formation, and intracellular calcium mobilization.
Keywords:Prostaglandin E1 receptor—Cyclic GMP—Cyclic AMP—Inositol phosphates—Intracellular calcium              Kanba S  et al  Two possibly distinct prostaglandin E1 receptors in N1E-115 clone: One mediating inositol trisphosphate formation  cyclic GMP formation  and intracellular calcium mobilization and the other mediating cyclic AMP formation
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