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Mechanisms of α-Sialosyl Cholesterol Action to Suppress Both Cyclic AMP Production and DNA Synthesis of Rat Glial Cells
Authors:Jin-ichi Ito  Taiji Kato  Ryo Tanaka
Institution:Department of Biochemistry, Nagoya City University Medical School, Nagoya, Japan;Department of Bioregulation Research, Nagoya City University Medical School, Nagoya, Japan
Abstract:Abstract: α-Sialosyl cholesterol (α-SC) that elicited morphological differentiation of rat astrocytes not only lowered intracellular cyclic AMP (cAMP) levels but also inhibited cAMP production induced by either α-isoproterenol, cholera toxin, or forskolin. The targets of α-SC in the cAMP production system of rat astrocytes were investigated to understand the mechanism of the a-SC action on cAMP production. cAMP production evoked by a-isoproterenol (1 μ M ) was entirely canceled by β blockers such as propranolol and timolol (1 μ M ), but not by α-SC. Concentrations of α-SC greater than 15 μ M were required for 50% inhibition of the activation by a β agonist. Although α-SC inhibited in a dose-dependent manner the activities of membrane-associated adenylate cyclase that had been stimulated by either GTPγS or forskolin, α-SC inhibited neither GTP-binding activities nor GTPase activities of the membrane-associated G proteins. These findings suggest that α-SC suppresses adenylate cyclase directly, but not β receptors or G proteins, and that it promotes the morphological differentiation of rat astrocytes through a mechanism regulating directly the cytoskeletal organization, regardless of intracellular cAMP level. α-SC (30 μ M ) suppressed 40% of DNA synthesis in the cell-free system, which contained the cytosolic extracts and the nucleus fraction prepared from rat astrocytoma C6 cells. Approximately 25% of α-SC incorporated in the astrocyte cytoplasm was transferred to the nuclei by 10 min after the addition. Thus, it is likely that α-SC that had been incorporated in the cytosol suppressed adenylate cyclase by acting from the cytosolic side of the plasma membrane, and separately suppressed nuclear DNA synthesis.
Keywords:α-Sialosyl cholesterol  Astrocyte  cAMP production  Adenylate cyclase  DNA inhibition
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