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依维莫司对维持期肾移植患者中环孢素稳态药代动力学的影响。

Influence of everolimus on steady-state pharmacokinetics of cyclosporine in maintenance renal transplant patients.

作者信息

Budde Klemens, Lehne Gustav, Winkler Michael, Renders Lutz, Lison Arno, Fritsche Lutz, Soulillou Jean-Paul, Fauchald Per, Neumayer Hans-Hellmut, Dantal Jaques

机构信息

University Clinic Charité, Berlin, Germany.

出版信息

J Clin Pharmacol. 2005 Jul;45(7):781-91. doi: 10.1177/0091270005277196.

Abstract

To investigate possible interactions of the novel immunosuppressant everolimus with cyclosporine, a multicenter, randomized, double-blind, placebo-controlled, dose-escalating phase I study was performed. Everolimus regimens (0.75-10 mg/d) were administered for 28 days to stable renal allograft recipients receiving the microemulsion form of cyclosporine. Steady-state cyclosporine profiles were assessed at baseline on day 0 (cyclosporine alone) and on day 21 with everolimus on steady state. By day 21, mean dose-normalized cyclosporine AUC0-12 increased by 15% in patients receiving placebo. In everolimus-treated patients, mean increases in cyclosporine AUC0-12 ranged from 7% to 43%, which were not significantly different across all dosing cohorts including placebo. Linear regression of everolimus AUC on day 21 versus the increase in cyclosporine AUC0-12 yielded a slope not significantly different from a horizontal line (P = ns). In conclusion, these results suggest that steady-state everolimus exposure over the wide range assessed in this study did not affect steady-state cyclosporine pharmacokinetics.

摘要

为研究新型免疫抑制剂依维莫司与环孢素之间可能的相互作用,开展了一项多中心、随机、双盲、安慰剂对照、剂量递增的I期研究。对接受环孢素微乳剂治疗的稳定肾移植受者给予依维莫司方案(0.75 - 10 mg/d),持续28天。在第0天(仅环孢素)基线时以及第21天依维莫司达稳态时评估环孢素的稳态情况。到第21天,接受安慰剂的患者中,平均剂量标准化的环孢素AUC0 - 12增加了15%。在接受依维莫司治疗的患者中,环孢素AUC0 - 12的平均增加幅度为7%至43%,在包括安慰剂在内的所有给药队列中差异均无统计学意义。第21天依维莫司AUC与环孢素AUC0 - 12增加量的线性回归得出的斜率与水平线无显著差异(P = 无显著性差异)。总之,这些结果表明,在本研究评估的广泛范围内,依维莫司的稳态暴露不影响环孢素的稳态药代动力学。

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