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尼鲁米特抑制未处理的雄性大鼠和人肝微粒体中乙苯妥英的4-羟基化反应。

Nilutamide inhibits mephenytoin 4-hydroxylation in untreated male rats and in human liver microsomes.

作者信息

Horsmans Y, Lannes D, Larrey D, Tinel M, Letteron P, Loeper J, Pessayre D

机构信息

Unité de Recherches de Physiopathologie Hépatique (INSERM U-24), Hôpital Beaujon, Clichy, France.

出版信息

Xenobiotica. 1991 Dec;21(12):1559-70. doi: 10.3109/00498259109044405.

Abstract
  1. The effects of nilutamide (an anti-androgen with a hydantoin moiety) on the 4-hydroxylation of mephenytoin were studied in rat liver microsomes. Nilutamide, at a concentration expected in human liver (100 microM) during prolonged administration of nilutamide, inhibited by 40% mephenytoin (0.3 mM) 4-hydroxylase activity in liver microsomes from untreated male rats, but not in microsomes from untreated female rats, or in microsomes from dexamethasone-treated male or female rats. 2. Administration to male rats of nilutamide, in doses (20 mg/kg i.p. twice daily) known to reproduce plasma concentrations observed in human therapeutics, decreased by 60% the 24 h urinary excretion of 4-hydroxymephenytoin after administration of mephenytoin (15 mg/kg oral). 3. Nilutamide (100 microM) markedly inhibited mephenytoin 4-hydroxylase activity in human liver microsomes. Inhibition kinetics were consistent with mixed inhibition. It is concluded that nilutamide inhibits mephenytoin 4-hydroxylase activity in untreated male rats and in human liver microsomes. It is suggested that inhibition is likely to occur in vivo in humans receiving therapeutic doses of nilutamide.
摘要
  1. 在大鼠肝微粒体中研究了尼鲁米特(一种含有乙内酰脲部分的抗雄激素药物)对美芬妥英4-羟基化作用的影响。在长期服用尼鲁米特期间,人肝脏中预期的浓度(100微摩尔/升)下,尼鲁米特抑制了未处理雄性大鼠肝微粒体中美芬妥英(0.3毫摩尔/升)4-羟化酶的活性达40%,但在未处理雌性大鼠的微粒体中,以及在地塞米松处理的雄性或雌性大鼠的微粒体中均未出现抑制作用。2. 以已知能重现人体治疗中观察到的血浆浓度的剂量(每天两次腹腔注射20毫克/千克)给雄性大鼠服用尼鲁米特,在口服美芬妥英(15毫克/千克)后,使4-羟基美芬妥英的24小时尿排泄量减少了60%。3. 尼鲁米特(100微摩尔/升)显著抑制人肝微粒体中美芬妥英4-羟化酶的活性。抑制动力学符合混合抑制。结论是,尼鲁米特抑制未处理雄性大鼠和人肝微粒体中美芬妥英4-羟化酶的活性。提示在接受治疗剂量尼鲁米特的人体中可能会在体内发生抑制作用。

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