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药物与大鼠体内异烟肼代谢的相互作用。

Drug interactions with isoniazid metabolism in rats.

作者信息

Thomas B H, Solomonraj G

出版信息

J Pharm Sci. 1977 Sep;66(9):1322-6. doi: 10.1002/jps.2600660930.

Abstract

14C-Isoniazid (20 mg/kg po or iv) was administered alone or in combination with aspirin (100 mg/kg po), rifampin (30 mg/kg po), ethambutol (100 mg/kg po), or ethanol (3 g/kg po) to rats. In another experiment, phenobarbital sodium (40 mg/kg/day ip) was administered for 3 days prior to isoniazid. Aspirin and ethanol retarted the rate of isoniazid absorption from the GI tract. None of the drugs significantly altered the 14C-elimination rate from the blood over the first 4 hr. A tissue distribution study showed that changes in the blood levels produced by ethanol were reflected in the other tissues. When isoniazid was given intravenously, ethanol increased the amount of carbon-14 excreted in urine up to 24 hr after dosing; no other changes were observed in the total carbon-14 recovered in urine. Aspirin inhibited the conjugation of isonicotinic acid with glycine. Ethanol increased N-acetylisoniazid excretion and decreased isonicotinic acid excretion. None of the other treatments had more than a slight effect on isoniazid metabolism. Acute doses of isoniazid failed to produce any signs of hepatotoxicity, as judged by measurement of serum transaminase levels. The data do not suggest that any of the drugs studied are likely to potentiate the hepatotoxicity of isoniazid when administered acutely. Isoniazid metabolism in rats differed quantitatively from that reported for humans.

摘要

将14C-异烟肼(20毫克/千克,口服或静脉注射)单独或与阿司匹林(100毫克/千克,口服)、利福平(30毫克/千克,口服)、乙胺丁醇(100毫克/千克,口服)或乙醇(3克/千克,口服)一起给予大鼠。在另一项实验中,在给予异烟肼前3天,腹腔注射苯巴比妥钠(40毫克/千克/天)。阿司匹林和乙醇延缓了异烟肼从胃肠道的吸收速率。在最初4小时内,没有一种药物能显著改变血液中14C的消除速率。一项组织分布研究表明,乙醇引起的血液水平变化反映在其他组织中。当静脉注射异烟肼时,乙醇使给药后24小时内尿中排出的碳-14量增加;在尿中回收的总碳-14中未观察到其他变化。阿司匹林抑制异烟酸与甘氨酸的结合。乙醇增加N-乙酰异烟肼的排泄并减少异烟酸的排泄。其他处理对异烟肼代谢的影响均不超过轻微程度。通过测量血清转氨酶水平判断,急性剂量的异烟肼未产生任何肝毒性迹象。数据表明,急性给药时,所研究的任何药物都不太可能增强异烟肼的肝毒性。大鼠体内异烟肼的代谢在数量上与人类报道的不同。

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