Your search keyword '"Kanba KS"' showing total 5 results

1. Desensitization of muscarinic M1 receptors of murine neuroblastoma cells (clone N1E-115) without receptor down-regulation and protein kinase C activity.

Author

Kanba S, Kanba KS, McKinney M, Pfenning M, Abraham R, Nomura S, Enloes L, Mackey S, and Richelson E

Subjects

Animals, Carbachol metabolism, Down-Regulation drug effects, Guanosine Monophosphate biosynthesis, Inositol Phosphates metabolism, Mice, N-Methylscopolamine, Neuroblastoma enzymology, Parasympatholytics metabolism, Receptors, Muscarinic metabolism, Scopolamine Derivatives metabolism, Tumor Cells, Cultured, Carbachol pharmacology, Neuroblastoma metabolism, Protein Kinase C metabolism, Receptors, Muscarinic drug effects, Tetradecanoylphorbol Acetate pharmacology

Abstract

Acute desensitization of M1 muscarinic receptor-mediated responses (cyclic GMP formation and inositol phosphate release) was studied in murine neuroblastoma cells (N1E-115 clone). After a 45-min incubation at 37 degrees of N1E-115 cells either in monolayer or in suspension, with the muscarinic agonist carbachol (1 mM), the receptor-mediated cyclic GMP response to carbachol was nearly completely lost. This loss was associated with greater than 80% loss of carbachol-mediated inositol phosphate release. The protein kinase C activator phorbol 12-myristate 13-acetate (PMA) inhibited both responses with similar potencies. Carbachol or PMA reduced by 30-40% the number of muscarinic receptor sites for antagonist and agonist on intact cells (determined in binding assays using [3H]N-methylscopolamine) only for cells in monolayer and not for those in suspension. PMA but not carbachol pretreatment of cells in monolayer or in suspension caused a translocation of [3H]phorbol 12,13-dibutyrate binding and protein kinase C activity. In addition, desensitization to carbachol occurred in cells largely depleted of protein kinase C by chronic exposure to PMA. Thus, agonist-mediated down-regulation is not needed for muscarinic M1 receptor desensitization, which may be a result of the activation of a receptor-activated kinase different from protein kinase C.

Published

1990

2. Neurotensin(8-13): comparison of novel analogs for stimulation of cyclic GMP formation in neuroblastoma clone N1E-115 and receptor binding to human brain and intact N1E-115 cells.

Author

Gilbert JA, McCormick DJ, Pfenning MA, Kanba KS, Enloe LJ, Moore A, and Richelson E

Subjects

Humans, Neuroblastoma metabolism, Neurotensin metabolism, Receptors, Neurotensin, Structure-Activity Relationship, Tumor Cells, Cultured, Brain metabolism, Cyclic GMP biosynthesis, Neurotensin pharmacology, Peptide Fragments pharmacology, Receptors, Neurotransmitter metabolism

Abstract

Neurotensin(8-13), the carboxyl-terminal portion of neurotensin, is 4-50 times more potent than native neurotensin in binding to intact neuroblastoma N1E-115 cells and human brain tissue and in stimulation of intracellular cyclic GMP production and inositol phospholipid hydrolysis in clone N1E-115 (Gilbert JA and Richelson E, Eur J Pharmacol 99: 245-246, 1984; Gilbert JA et al., Biochem Pharmacol 35: 391-397, 1986; Kanba KS et al., J Neurochem 46: 946-952, 1986; and Kanba KS and Richelson E, Biochem Pharmacol 36: 869-874, 1987). A series of novel analogs of neurotensin (8-13) was synthesized, and a structure-activity study was done comparing the abilities of these peptides to stimulate intracellular cyclic GMP production in intact neuroblastoma clone N1E-115 and to inhibit the binding of [3H]neurotensin to these cells and to membranal preparations from human brain. A direct correlation was found for each analog between its EC50 for biochemical activity and its KD for binding ability in studies with clone N1E-115. Furthermore, a strong correlation existed for each peptide between its KD for binding to neurotensin receptors on these cells and its KD for binding to neurotensin receptors in human brain tissue. In this study, the residues that were important to the biochemical and binding activities of neurotensin (8-13) proved to be identical to the amino acids that are necessary for the functional integrity of native neurotensin (Gilbert JA et al., Biochem Pharmacol 35: 391-397, 1986.

Published

1989

3. Lithium ions have a potent and selective inhibitory effect on cyclic GMP formation stimulated by neurotensin, angiotensin II and bradykinin.

Author

Kanba S, Pfenning M, Kanba KS, and Richelson E

Subjects

Animals, Cells, Cultured, Mice, Phosphodiesterase Inhibitors, Angiotensin II pharmacology, Bradykinin pharmacology, Cyclic GMP biosynthesis, Lithium pharmacology, Neurotensin pharmacology

Abstract

The effect of lithium ion (Li+) on receptor-mediated synthesis of cyclic GMP, a putative second messenger, was examined using intact murine neuroblastoma cells (clone N1E-115). Lithium chloride potently inhibited cyclic GMP formation stimulated by the neuropeptides, neurotensin, angiotensin II and bradykinin in an identical concentration-dependent (IC50 s of around 12 mM), saturable and reversible manner. In the presence of veratridine, an alkaloid which by stimulating sodium channels can increase Li+ entry into the cells, Li+ inhibited neurotensin-stimulated cyclic GMP formation more potently (IC50 = 7 mM). No effect of Li+ was observed on phosphodiesterase (EC 3.1.4.17) activity. These results suggest that Li+ may interfere with the function of these receptors through its inhibitory effect at a common site in the pathway of receptor-mediated cyclic GMP formation.

Published

1986

4. The protein kinase C activator, 12-O-tetradecanoylphorbol-13-acetate (TPA), inhibits muscarinic (M1) receptor-mediated inositol phosphate release and cyclic GMP formation in murine neuroblastoma cells (clone N1E-115).

Author

Kanba S, Kanba KS, and Richelson E

Subjects

Animals, Carbachol pharmacology, Cell Line, Mice, Neuroblastoma, Phorbol Esters pharmacology, Cyclic GMP biosynthesis, Inositol Phosphates metabolism, Phorbols pharmacology, Protein Kinase C metabolism, Receptors, Muscarinic drug effects, Sugar Phosphates metabolism, Tetradecanoylphorbol Acetate pharmacology

Published

1986

5. Comparison of the stimulation of inositol phospholipid hydrolysis and of cyclic GMP formation by neurotensin, some of its analogs, and neuromedin N in neuroblastoma clone N1E-115.

Author

Kanba KS and Richelson E

Subjects

Animals, Cell Line, Inositol Phosphates metabolism, Mice, Neurotensin analogs & derivatives, Cyclic GMP biosynthesis, Neuroblastoma metabolism, Neurotensin pharmacology, Peptide Fragments pharmacology, Phosphatidylinositols metabolism

Abstract

Neurotensin, some of its analogs, and neuromedin N were examined for comparison of their potencies at stimulating inositol phospholipid hydrolysis and cyclic GMP synthesis in intact murine neuroblastoma cells (clone N1E-115). Neurotensin(8-13) and acetylneurotensin(8-13) had the highest potencies for the stimulation of the hydrolysis of inositol phospholipid, which were about three times as potent as neurotensin (EC50 = 0.9 nM). On the other hand, fragments of the amino-terminal portion of neurotensin, such as neurotensin(1-6), neurotensin(1-8) and neurotensin(1-11), showed no ability to stimulate this hydrolysis. Neuromedin N, which is similar in structure to neurotensin(8-13) and which has been demonstrated to stimulate cyclic GMP formation [J.A. Gilbert and E. Richelson, Eur. J. Pharmac. 129, 379 (1986)], had EC50 values of 2.5 and 4.5 nM for release of [3H]inositol phosphates and stimulation of cyclic [3H]GMP respectively. A strong correlation was obtained between the EC50 values for neurotensin and several analogs in the stimulation of the release of inositol phosphates and the EC50 values for these peptides in the stimulation of cyclic GMP formation in neuroblastoma clone N1E-115 cells under similar experimental conditions. Thus, these two different biochemical effects of neurotensin and its analogs appear to be mediated by the same receptor site, which may also have been the site of action of neuromedin N in these cells.

Published

1987