Chronotoxicity of Methotrexate in Mice and Its Relation to Circadian Rhythm of DNA Synthesis and Pharmacokinetics
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概要
- 論文の詳細を見る
The mechanisms underlying the circadian rhythm of methotrexate (MTX)-induced toxicity (body weight loss and leukopenia) were investigated from the viewpoints of the sensitivity of living organisms to the drug and the pharmacokinetics of the drug. ICR male mice were housed in a standardized light-dark cycle (lights on at 0700, off at 1900) with food and water ad libitum. The body weight loss after an intraperitoneal injection of MTX (400 mg/kg) was more serious in the late dark period and the early light period and milder in the late light period and the early dark period. The MTX-induced leukopenia was more serious in the late dark period and the light period and milder in the early dark period. Lower toxicity was observed when DNA synthesis, dihydrofolate reductase (DHFR) activity in bone marrow cells and folate level in plasma decreased, and higher toxicity was observed when they increased. There was a significant circadian rhythm in plasma MTX concentration, with a higher level in the light period and a lower level in the dark period. The circadian rhythm of plasma MTX concentration was associated with that of MTXinduced toxicity. The present study suggests that the circadian rhythm of MTX-induced toxicity is caused by that of the sensitivity of living organisms to the drug and the pharmacokinetics of the drug.
- 社団法人 日本薬理学会の論文
- 1997-11-01
著者
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YUKAWA Eiji
Department of Clinical Pharmacokinetics, Daiichi University, College of Pharmaceutical Sciences
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HIGUCHI Shun
Department of Clinical Pharmacokinetics, Graduate School, Kyushu University
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NAKANO Shigeyuki
大分医科大学臨床薬理学
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Nakano Shigeyuki
Department Of Pharmaceutical Medicine Oita University Faculty Of Medicine
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Nakano Shigeyuki
Department Of Clinical Pharmacology And Therapeutics Oita Medical University
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INOUE KOUICHI
Department of Surgery, School of Medicine, Showa University
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OHDO Shigehiro
Department of Pharmaceutics, Division of Pharmaceutical Science, Graduate School, Kyushu University
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Ogawa Nobuya
Department Of Pharmacology Ehime University School Of Medicine
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Ogawa Nobuya
Department Of Clinical Pharmacology Ehime University School Of Medicine
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Ohdo Shigehiro
Pharmaceutics Division Of Clinical Pharmacy Department Of Medico-pharmaceutical Science Faculty Of P
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Ohdo Shigehiro
Department Of Pharmaceutics Division Of Pharmaceutical Science Graduate School Kyushu University
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YUKAWA Eiji
Division of Pharmaceutical Sciences, Kyushu University
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Yukawa Eiji
Clinical Pharmacokinetics Division Of Clinical Pharmacy Department Of Medico-pharmaceutical Sciences
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Yukawa Eiji
Department Of Clinical Pharmacokinetics Daiichi University College Of Pharmaceutical Sciences
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Higuchi Shun
Department Of Clinical Pharmacokinetics Graduate School Kyushu University
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Higuchi Shun
Department Of Clinical Pharmacokinetics Division Of Pharmaceutical Sciences Kyushu University
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Ohdo Shigehiro
Department Of Clinical Pharmacokinetics Division Of Pharmaceutical Sciences Kyushu University
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Inoue K
Pharmaceutics Division Of Clinical Pharmacy Department Of Medico-pharmaceutical Science Faculty Of P
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Inoue Kouichi
Department Of Mathematics Faculty Of Science Kyoto University
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OGAWA Nobuya
Department of Pharmacology, Ehime University School of Medicine
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INOUE Kouichi
Department of Bioscience Development, School of Bioscience, Hiroshima Prefectural University
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