Effects of twenty-three drugs on the metabolism of FK506 by human liver microsomes.

K Iwasaki, H Matsuda, K Nagase, T Shiraga, Y Tokuma, K Uchida
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Abstract

We investigated the effects of 23 drugs on the metabolism of FK506 by human liver microsomes. Acyclovir, amphotericin B, cefixime, cefotaxime, ciprofloxacin, cyclosporin A, diltiazem, enoxacin, erythromycin, ethinyl estradiol, fluconazole, fosfomycin, kanamycin, lincomycin, loxoprofen, minocyclin, nifedipine, nilvadipine, norethindrone, ofloxacin, phenobarbital, prednisolone, or rifampicin was added to the reaction media at equimolar or at ten times an excess molar ratio of the substrate concentration; their effects on FK506 metabolism were examined. Drugs known to be the substrate of cytochrome P-450 3A inhibited the metabolism of FK506, and among the drugs tested, the inhibition by cyclosporin A and nifedipine was the strongest.

23种药物对人肝微粒体代谢FK506的影响。
我们研究了23种药物对人肝微粒体代谢FK506的影响。将阿昔洛韦、两性霉素B、头孢克肟、头孢噻肟、环丙沙星、环菌素A、地尔硫卓、依诺沙星、红霉素、炔雌醇、氟康唑、磷霉素、卡那霉素、林可霉素、洛索洛芬、米诺环素、硝苯地平、尼伐地平、去瑞辛酮、氧氟沙星、苯巴比妥、强的松龙或利福平以等摩尔或十倍的底物浓度添加到反应介质中;检测其对FK506代谢的影响。已知为细胞色素p - 4503a底物的药物可抑制FK506的代谢,在所测药物中,环孢素A和硝苯地平的抑制作用最强。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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