Spoendlin M, Peters J, Welker H, Bock A, Thiel G
Division of Nephrology, University of Basel, Kantonsspital, Switzerland.
Nephrol Dial Transplant. 1998 Jul;13(7):1787-91. doi: 10.1093/ndt/13.7.1787.
The potential for interaction between oral cyclosporin (Sandimmun) and the new calcium antagonist mibefradil was assessed as part of the clinical development of the new compound.
Six stable renal transplant patients on long-term, oral, twice-daily (Q 12 H) cyclosporin (CsA) therapy received 25 mg mibefradil on Day 1, followed by 50 mg once daily for 5 or 6 days. At baseline, as well as on the last day of mibefradil dosing, complete steady-state CsA blood concentration-time profiles were characterized over a dosing interval.
Mibefradil led to mean increases in minimum and maximum CsA blood concentrations and area under the curve of CsA by 2.7-, 2.1-, and 2.3-fold, respectively (all significantly different from CsA alone, P < 0.02). Mibefradil is therefore associated with a clinically relevant increase in CsA blood concentrations. The mechanism of elevation of CsA blood concentrations is probably mibefradil and/or metabolite inhibition of the cytochrome P-450 isoenzyme 3A4. CsA had no clinically significant effect on mibefradil plasma concentrations.
These results confirm previous findings of cytochrome P-450 3A4 inhibition by mibefradil and suggest that, for patients receiving CsA, its dose must be adjusted and its plasma concentration must be monitored when adding or stopping mibefradil.
作为新化合物临床开发的一部分,评估了口服环孢素(山地明)与新型钙拮抗剂米贝拉地尔之间相互作用的可能性。
6例接受长期口服、每日两次(每12小时一次)环孢素(CsA)治疗的稳定肾移植患者,在第1天服用25mg米贝拉地尔,随后5或6天每日服用50mg。在基线以及米贝拉地尔给药的最后一天,在一个给药间隔内对完整的稳态CsA血药浓度-时间曲线进行表征。
米贝拉地尔使CsA的最低和最高血药浓度以及CsA曲线下面积分别平均增加2.7倍、2.1倍和2.3倍(均与单独使用CsA有显著差异,P<0.02)。因此,米贝拉地尔与CsA血药浓度的临床相关升高有关。CsA血药浓度升高的机制可能是米贝拉地尔和/或其代谢产物对细胞色素P-450同工酶3A4的抑制。CsA对米贝拉地尔血浆浓度无临床显著影响。
这些结果证实了先前关于米贝拉地尔抑制细胞色素P-450 3A4的发现,并表明,对于接受CsA治疗的患者,在加用或停用米贝拉地尔时,必须调整其剂量并监测其血浆浓度。
