Li R C, Narang P K, Sahai J, Cameron W, Bianchine J R
Department of Pharmacy, Faculty of Medicine, The Chinese University of Hong Kong, Shatin.
Antimicrob Agents Chemother. 1997 Jul;41(7):1566-70. doi: 10.1128/AAC.41.7.1566.
Didanosine (ddI) is currently used in the management of patients infected by the human immunodeficiency virus. Rifabutin (RBT) is being extensively used for prophylaxis against Mycobacterium avium complex (MAC) infections. Due to its acid-labile characteristics, ddI must be administered with a buffer. Recent reports have indicated that absorption of ketoconazole, ciprofloxacin, and dapsone, etc., in the gut is altered by concomitant ddI dosing. We have assessed whether concomitant dosing of ddI as antiretroviral therapy modifies RBT absorption in the gut, its steady-state pharmacokinetics, and/or safety in 15 patients with AIDS. Of the 15 patients enrolled, 12 completed the study and 3 receiving 600 mg of RBT with concomitant ddI administration withdrew prematurely from the study. Steady-state RBT pharmacokinetics were assessed on day 13 (ddI plus RBT) and day 16 (RBT alone). The ddI doses (adjusted for body weight) were 167 to 375 mg twice daily, while RBT was administered as a single 300- or 600-mg daily dose. No statistically significant (P > 0.05) differences were seen in RBT absorption parameter estimates between days 13 and 16: maximum concentration in plasma (Cmax; 511 +/- 341 ng/ml versus 525 +/- 254 ng/ml) and the time at which Cmax was observed (3.0 versus 2.5 h). The mean RBT estimates for area under the concentration-time curve from 0 to 24 h (AUC(0-tau)) (5,650 versus 5,023 ng x h/ml) and for oral clearance (1.28 versus 1.18 liter/h/kg) on both study days were also similar. Assessment based on urinary recovery of RBT (3.1 versus 3.7 mg) and its predominant deacetyl metabolite, LM565 (1.6 versus 1.4 mg), showed no apparent effect of ddI. The fraction of the RBT dose converted to LM565, as suggested by the ratio of AUC of the metabolite to AUC of the parent drug, was also unaltered (0.15 versus 0.12). A ratio analysis (day 13/day 16) of the RBT pharmacokinetic estimates showed that the 95% confidence intervals for all parameters were inclusive of one. Furthermore, the brief interruption of ddI therapy over this short study period at steady state produced no clinically significant changes in body weight, hematology, and renal and pancreatic functions. Therefore, concomitant administration of ddI appears not to affect RBT absorption in the gut and its disposition or safety in patients with AIDS.
去羟肌苷(ddI)目前用于治疗人类免疫缺陷病毒感染患者。利福布汀(RBT)被广泛用于预防鸟分枝杆菌复合体(MAC)感染。由于其酸不稳定特性,ddI必须与缓冲剂一起给药。最近的报告表明,同时服用ddI会改变酮康唑、环丙沙星和氨苯砜等在肠道的吸收。我们评估了在15例艾滋病患者中,将ddI作为抗逆转录病毒疗法同时给药是否会改变RBT在肠道的吸收、其稳态药代动力学和/或安全性。在纳入的15例患者中,12例完成了研究,3例在接受600mg RBT并同时服用ddI时提前退出了研究。在第13天(ddI加RBT)和第16天(单独服用RBT)评估了RBT的稳态药代动力学。ddI剂量(根据体重调整)为每日两次,每次167至375mg,而RBT作为每日一次300mg或600mg的单剂量给药。在第13天和第16天之间,RBT吸收参数估计值没有统计学上的显著差异(P>0.05):血浆中的最大浓度(Cmax;511±341ng/ml对525±254ng/ml)以及观察到Cmax的时间(3.0对2.5小时)。在两个研究日,0至24小时浓度-时间曲线下面积(AUC(0-tau))(5650对5023ng·h/ml)和口服清除率(1.28对1.18升/小时/千克)的RBT平均估计值也相似。基于RBT的尿回收率(3.1对3.7mg)及其主要脱乙酰代谢产物LM565(1.6对1.4mg)的评估显示,ddI没有明显影响。代谢产物AUC与母体药物AUC之比表明,转化为LM565的RBT剂量分数也未改变(0.15对0.12)。RBT药代动力学估计值的比率分析(第13天/第16天)表明,所有参数的95%置信区间都包含1。此外,在这个短研究期的稳态下短暂中断ddI治疗,在体重、血液学以及肾脏和胰腺功能方面没有产生临床显著变化。因此,同时给予ddI似乎不会影响RBT在肠道的吸收及其在艾滋病患者中的处置或安全性。
