FK 506 (Tacrolimus) metabolism by rat liver microsomes and its inhibition by other drugs.

T N Prasad, D D Stiff, N Subbotina, M A Zemaitis, G J Burckart, T E Starzl, R Venkataramanan
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Abstract

The in vitro metabolism of FK 506 and its inhibition by other drugs was studied with hepatic microsomes from rats pre-treated with dexamethasone, a selective cytochrome P-450 IIIA inducer. Nonspecific inhibitors of cytochrome P-450, such as ketoconazole, itraconazole, fluconazole and SKF 525 A, and most of the cytochrome P-450 IIIA specific substrates used in this study significantly inhibited FK 506 metabolism. Although cyclosporine is a known substrate of cytochrome P-450 IIIA, it had no effect on FK 506 metabolism. Cytochrome P-450 II substrates had minimal but significant effect on FK 506 metabolism. This data supports our earlier observations that FK 506 metabolism is mediated predominantly by the steroid inducible cytochrome P-450 IIIA enzyme subfamily. The results of this study indicate that in transplant patients there is a potential for an interaction of FK 506 with other drugs that are metabolized by the cytochrome P-450 IIIA subfamily or those that alter the activity of cytochrome P-450 IIIA subfamily. Careful monitoring and FK 506 dosing adjustment may be necessary to maintain therapeutic concentration and minimize toxicity in patients receiving this agent.

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大鼠肝微粒体对fk506(他克莫司)的代谢及其对其他药物的抑制作用。
采用选择性细胞色素P-450 IIIA诱导剂地塞米松预处理大鼠肝微粒体,研究fk506体外代谢及其对其他药物的抑制作用。细胞色素P-450的非特异性抑制剂,如酮康唑、伊曲康唑、氟康唑和SKF 525a,以及本研究中使用的大多数细胞色素P-450 IIIA特异性底物均可显著抑制fk506代谢。虽然环孢素是已知的细胞色素P-450 IIIA的底物,但它对fk506的代谢没有影响。细胞色素P-450 II底物对fk506代谢的影响虽小但显著。这一数据支持了我们早期的观察,即fk506代谢主要由类固醇诱导的细胞色素P-450 IIIA酶亚家族介导。本研究结果表明,在移植患者中,fk506可能与其他被细胞色素P-450 IIIA亚家族代谢的药物或改变细胞色素P-450 IIIA亚家族活性的药物相互作用。仔细的监测和fk506的剂量调整可能是必要的,以维持治疗浓度,并尽量减少服用该药物的患者的毒性。
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