Studies on Somnolence in the Daytime Caused by Drugs Used for Neuropathic Pain
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概要
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In the present study, the characteristics of the sleep features of amitriptyline, mexiletine, and N-(4-tertiarybutylphenyl)-4-(3-cholorphyridin-2-yl)tetrahydropyradine-1(2H)-carbox-amide (BCTC) were studied. Electrodes were chronically implanted into the frontal cortex and the dorsal neck muscles of rats for electroencephalogram (EEG) and electromyogram (EMG) measurements, respectively. EEG and EMG were recorded with an electroencephalograph, and SleepSign ver. 2.0. was used for sleep–wake state analysis. Recordings were performed from 11:00 to 17:00. Amitriptyline caused significant decreases in sleep latency and total wake time and an increase in total non-rapid eye movement (non-REM) sleep time. Mexiletine caused a significant decrease in sleep latency, but no significant effect was observed in total wake time and total non-REM sleep time. On the other hand, BCTC, which is an antagonist of transient receptor potential vaniloid 1 (TRPV1), showed no significant effect on sleep latency, total wake time, total non-REM sleep time, and total REM sleep time. From these results, it can be concluded that a TRPV1 antagonist may become a useful drug for neuropathic pain without sedative side effects in the daytime, different from amitriptyline and mexiletine.
- 社団法人 日本薬理学会の論文
- 2008-07-20
著者
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Kamei Chiaki
Department of Medicinal Pharmacology, Okayama University Graduate School of Medicine, Dentistry and
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Takeda Yasuhiro
Department of Life and Materials Engineering, Nagoya Institute of Technology
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ISHIDA Takayuki
Department of Applied Physics and Chemistry, The University of Electro-Communications
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Kamei Chiaki
Dep. Of Medicinal Pharmacology Okayama Univ. Graduate School Of Medicine Dentistry And Pharmaceutica
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Kamei Chiaki
Department Of Medicinal Pharmacology Okayama University Graduate School Of Medicine Dentistry And Ph
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Tanimoto Mori
Pfizer Global Research And Development Nagoya Laboratories Pfizer Inc.
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TSUTSUI Ryuki
Department of Medicinal Pharmacology, Okayama University Graduate School of Medicine, Dentistry and
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TOIDE Katsuo
Pfizer Global Research and Development, Nagoya Laboratories, Pfizer Inc.
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WATANABE Shuzo
Pfizer Global Research and Development, Nagoya Laboratories, Pfizer Inc.
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KANAI Yoshihito
Pfizer Global Research and Development, Nagoya Laboratories, Pfizer Inc.
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Ishida Takayuki
Department Of Applied Pharmacology Kagoshima University Graduate School Of Medical And Dental Scienc
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Takeda Yasuhiro
Department Of Medicinal Pharmacology Okayama University Graduate School Of Medicine Dentistry And Ph
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Takeda Yasuhiro
Department Of Animal Science Utsunomiya University
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Kanai Yoshihito
Department Of Pharmaceutical Care And Health Sciences Okayama University Graduate School Of Medicine
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Kitamura Yoshihisa
Department Of Neurobiology Kyoto Pharmaceutical University
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Kitamura Yoshihisa
Department Of Neuropharmacology Faculty Of Pharmaceutical Sciences Fukuoka University
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Kitamura Y
Department Of Neurobiology Kyoto Pharmaceutical University
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Kitamura Y
Shimizu Pharmaceutical Co. Ltd. Shizuoka Jpn
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Watanabe Shuzo
Pfizer Global Research And Development Nagoya Laboratories Pfizer Inc.
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Toide Katsuo
Pfizer Global Research And Development Nagoya Laboratories Pfizer Inc.
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Kamei Chiaki
Department Of Medical Pharmacology Okayama University Graduate School Of Medicine Dentistry And Phar
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Kamei Chiaki
Dep. Of Medicinal Pharmacology Okayama Univ. Graduate School Of Medicine Dentistry And Pharmaceutica
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Kamei Chiaki
Department Of Medicinal Pharmacology Okayama University Graduate School Of Medicine Dentistry And Ph
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Ishida Takayuki
Department of Medicinal Pharmacology, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences
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Tsutsui Ryuki
Department of Medicinal Pharmacology, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences
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