Activation of Cerebral Function by CS-932, a Functionally Selective M_1 Partial Agonist : Neurochemical Characterization and Pharmacological Studies
スポンサーリンク
概要
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A newly synthesized agonist for muscarinic acetylcholine (ACh) receptors CS-932, (R)-3-(3-isoxazoloxy)-1-azabicyclo-[2.2.2] octane hydrochloride, showed a relatively higher affinity for M1 than M2 receptors expressed in Chinese hamster ovary (CHO)-cells in comparison with ACh. CS-932 elevated the intracellular Ca2+ level only in M1-CHO cells, although ACh increased the level in both M1- and M3-CHO cells. CS-932 and ACh reduced forskolin-stimulated accumulation of cAMP in M2-CHO cells by 20% and 80%, respectively. This neurochemical profile of CS-932 indicates that the compound can activate M1-receptor-mediated functions selectively. CS-932 increased firing of cholinoceptive neurons in rat hippocampal slices, and this excitation was antagonized by pirenzepine, but not by AF-DX116. CS-932 increased awake and decreased slow wave sleep episodes of daytime EEG in free-moving rats. It counteracted scopolamine-induced slow waves in rat cortical EEG. CS-932 also increased the power of α- and β-waves, but decreased δ-wave of the cortical EEG in anesthetized monkeys. It ameliorated scopolamine-induced impairment of working memory in rats. Orally administered CS-932 had the best penetration into the brain among the muscarinic agonists tested and caused the least salivary secretion among the cholinomimetics examined. These results indicate that CS-932 has potential as a cognitive enhancer with fewer side effects in therapy for Alzheimer disease.
- 2000-11-01
著者
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YAMAMOTO Tsuneyuki
Department of Pharmacology, Graduate School of Pharmaceutical Sciences, Kyushu University
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Sakai J
Toyama Univ. Toyama
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Sakai Jun-ichi
Laboratory For Plasma Astrophysics Faculty Of Engineering Toyama University
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Sakai J
Laboratory For Plasma Astrophysics Faculty Of Engineering Toyama University
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Yamamoto Tsuneyuki
Department Of Pharmacology Graduate School Of Pharmaceutical Sciences Kyushu University
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Hara Takao
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Kaneko Tsugio
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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IWATA Nobuyoshi
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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KOZUKA Masao
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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TONOHIRO Toshiyuki
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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SUGIMOTO Masahiko
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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NIITSU Yoichi
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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KONDO Yusuke
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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SAKAI Jun-ichi
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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NAGANO Mitsuo
Neuroscience and Immunology Research Laboratories, Sankyo Co., Ltd.
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Hara T
Department Of Environmental Physiology Faculty Of Medicine Shimane University
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Kozuka Masao
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Kozuka Masao
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd
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Nagano Mitsuo
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Iwata Nobuyoshi
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Sugimoto M
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Tonohiro Toshiyuki
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Yamamoto Tsuneyuki
Department Of Developmental Biology Of Hard Tissue Graduate School Of Dental Medicine Hokkaido Unive
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Niitsu Yoichi
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Kondo Yusuke
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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Sakai Jun-ichi
Neuroscience And Immunology Research Laboratories Sankyo Co. Ltd.
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