环孢素与伊曲康唑在肾移植受者中的有益药代动力学相互作用。
Beneficial pharmacokinetic interaction between cyclosporine and itraconazole in renal transplant recipients.
作者信息
Florea N R, Capitano B, Nightingale C H, Hull D, Leitz G J, Nicolau D P
机构信息
Department of Pharmacy Practice, Loma Linda University School of Pharmacy, Loma Linda, California, USA.
出版信息
Transplant Proc. 2003 Dec;35(8):2873-7. doi: 10.1016/j.transproceed.2003.10.058.
BACKGROUND
Itraconazole is often given for fungal prophylaxis to renal transplant recipients, who require concomitant cyclosporine in the immediate posttransplant period. We determined the extent of the pharmacokinetic interaction between cyclosporine and itraconazole oral solution in renal transplant recipients and the effect on daily drug costs.
METHOD
This was a single-center, open-label, nonrandomized study. Posttransplantation, renal transplant recipients received itraconazole solution 200 mg twice daily and cyclosporine, dosed to achieve target concentrations. Once at steady state, blood samples were collected over 12 hours for pharmacokinetic evaluation of cyclosporine, itraconazole, and hydroxy-itraconazole. Itraconazole was discontinued after approximately a 3-month prophylaxis regimen. Cyclosporine doses were titrated to achieve target concentrations and cyclosporine concentrations were once again determined when steady state was achieved. A noncompartmental analysis was used to analyze cyclosporine pharmacokinetic parameters. The pharmacoeconomic impact was measured based on the percent change in dose of cyclosporine when administered with and without itraconazole. Drug costs were calculated using the average wholesale price. The cost per patient, as well as the average cost, was calculated for the cyclosporine/itraconazole combination, as well as the cyclosporine regimen alone.
RESULTS
Eight renal transplant recipients completed the study. All were included for itraconazole analyses and seven for cyclosporine analyses. Mean peak and trough itraconazole levels were 1.64 +/- 0.82 and 1.23 +/- 0.90 microg/mL respectively. Mean peak and trough hydroxy-itraconazole levels were 2.37 +/- 1.55 and 2.20 +/- 1.48 microg/mL, respectively. While on itraconazole, a 48% reduction in the mean total daily dose of cyclosporine was necessary to maintain target concentrations (171 +/- 63.6 versus 329 +/- 103.5 mg, P =.003). This reduction in cyclosporine dose resulted in a discounted itraconazole daily drug cost of approximately 29.5%.
CONCLUSION
Administering itraconazole with cyclosporine allows for a decrease in the cyclosporine dose, thus lowering daily drug costs and providing adequate antifungal coverage with itraconazole and hydroxy-itraconazole trough concentrations above the MIC(90) of Candida and Aspergillus spp.
背景
伊曲康唑常用于肾移植受者的真菌预防,这些患者在移植后即刻需要同时使用环孢素。我们确定了肾移植受者中环孢素与伊曲康唑口服溶液之间药代动力学相互作用的程度以及对每日药物费用的影响。
方法
这是一项单中心、开放标签、非随机研究。肾移植受者在移植后接受每日两次200mg伊曲康唑溶液和环孢素治疗,根据目标浓度调整环孢素剂量。达到稳态后,在12小时内采集血样,用于环孢素、伊曲康唑和羟基伊曲康唑的药代动力学评估。在大约3个月的预防疗程后停用伊曲康唑。调整环孢素剂量以达到目标浓度,达到稳态后再次测定环孢素浓度。采用非房室分析来分析环孢素的药代动力学参数。基于联用和不联用伊曲康唑时环孢素剂量的百分比变化来衡量药物经济学影响。使用平均批发价计算药物费用。计算环孢素/伊曲康唑联合用药以及单独使用环孢素方案时每位患者的费用以及平均费用。
结果
8名肾移植受者完成了研究。所有患者均纳入伊曲康唑分析,7名纳入环孢素分析。伊曲康唑的平均峰浓度和谷浓度分别为1.64±0.82和1.23±0.90μg/mL。羟基伊曲康唑的平均峰浓度和谷浓度分别为2.37±1.55和2.20±1.48μg/mL。在使用伊曲康唑期间,为维持目标浓度,环孢素的平均每日总剂量需降低48%(171±63.6mg对329±103.5mg,P = 0.003)。环孢素剂量的降低使伊曲康唑的每日药物费用降低了约29.5%。
结论
伊曲康唑与环孢素联用可降低环孢素剂量,从而降低每日药物费用,并使伊曲康唑和羟基伊曲康唑的谷浓度高于念珠菌和曲霉属的MIC(90),提供足够的抗真菌覆盖。
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