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补骨脂素对药物代谢的抑制与诱导作用:对戊巴比妥诱导的小鼠睡眠时间以及咖啡因和戊巴比妥在小鼠体内清除率的影响。

Inhibition and induction of drug metabolism by psoralens: alterations in duration of sleep induced by hexobarbital and in clearance of caffeine and hexobarbital in mice.

作者信息

Apseloff G, Hilliard J B, Gerber N, Mays D C

机构信息

Department of Pharmacology, College of Medicine, Ohio State University, Columbus.

出版信息

Xenobiotica. 1991 Nov;21(11):1461-71. doi: 10.3109/00498259109044396.

Abstract
  1. Hexobarbital (100 mg/kg i.p.) sleeping times in male CD-1 mice pretreated (-1 h) with a single i.p. injection of 150 mumol/kg of psoralen or coumarin analogues were increased, most markedly (6-fold) by linear, methoxy-substituted psoralens. 2. Hexobarbital sleeping times of mice which received three daily injections (231 mumol/kg; 50 mg/kg) of 8-methoxypsoralen (8-MOP) were 44% of controls (corn oil). 3. The whole-body half-life of caffeine (1 mg) in mice was 10.2, 1.2, and 0.37 h following 8-MOP (50 mg/kg per day) x 1, vehicle, and 8-MOP x 3 respectively. 4. The whole-body concentrations of hexobarbital (100 mg/kg dose) in mice 30 min after dosing were 14.3 +/- 0.9, 8.4 +/- 0.3, and 5.2 +/- 0.5 micrograms/ml (1 mouse = 150 ml) following 8-MOP (50 mg/kg per day) x 1, vehicle, and 8-MOP x 3 respectively. 5. It is concluded that, administered acutely, psoralen analogues inhibit hexobarbital metabolism in mice; and 8-MOP administered acutely inhibits the metabolism of caffeine and hexobarbital, but administered repeatedly increases their metabolism.
摘要
  1. 用150μmol/kg补骨脂素或香豆素类似物单次腹腔注射预处理(-1小时)的雄性CD-1小鼠,己巴比妥(100mg/kg腹腔注射)睡眠时间延长,其中线性甲氧基取代补骨脂素的延长最为显著(6倍)。2. 每天注射三次(231μmol/kg;50mg/kg)8-甲氧基补骨脂素(8-MOP)的小鼠,己巴比妥睡眠时间为对照组(玉米油)的44%。3. 咖啡因(1mg)在小鼠体内的全身半衰期,在8-MOP(50mg/kg/天)单次注射、溶剂对照和8-MOP三次注射后分别为10.2、1.2和0.37小时。4. 给药30分钟后,小鼠体内己巴比妥(100mg/kg剂量)的全身浓度,在8-MOP(50mg/kg/天)单次注射、溶剂对照和8-MOP三次注射后分别为14.3±0.9、8.4±0.3和5.2±0.5μg/ml(1只小鼠=150ml)。5. 得出的结论是,急性给药时,补骨脂素类似物抑制小鼠体内己巴比妥的代谢;急性给药的8-MOP抑制咖啡因和己巴比妥的代谢,但重复给药会增加它们的代谢。

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