Jacqz-Aigrain E, Khan Shaghaghi E, Baudouin V, Popon M, Zhang D, Maisin A, Loirat C
Unité de Pharmacologie Clinique Pédiatrique, Hôpital Robert Debré, 48 Boulevard Sérurier, F-75019 Paris, France.
Pediatr Nephrol. 2000 Feb;14(2):95-9. doi: 10.1007/s004670050020.
Mycophenolate mofetil (MMF) is a prodrug that is hydrolyzed to the active immunosuppressant mycophenolic acid (MPA). The drug is now widely prescribed for adult renal transplant recipients and its use has been extended to pediatric patients, although pharmacological data in this age group are limited. Nine pediatric renal transplant recipients received MMF with corticosteroids and either cyclosporine or tacrolimus a median of 55 months (range 7.5-124 months) months after transplantation. The pharmacokinetic parameters of MPA and MPA glucuronide (MPAG) were determined at steady state by high-performance liquid chromatography after administration of MMF at the oral dose of 494+/-142 mg/m(2) twice daily. MPA was rapidly absorbed, with a peak concentration at 1.4 h. The mean plasma concentration of MPA at steady state was 4.7+/-1.3 microg/ml. The areas under the plasma concentration-time curves (AUCs) over 12 h (between two administrations) were 57.0+/-15.3 microg.h/ml for MPA and 1,515+/-722 microg.h/ml for MPAG, and the apparent oral clearance was 11.7+/-7.0 and 0.5+/-0.4 l/h for MPA and MPAG, respectively. Assuming that the pharmacokinetics of MPA was dose dependent, the mean concentration at steady state and the AUC for MPA were calculated for the recommended dosage schedule of 600 mg/m(2) every 12 h and were 6.3+/-2.7 microg/ml and 75.2+/-32.9 microg.h/ml, respectively. The tolerance of MMF was studied prospectively with a follow-up of 1.1+/-0.2 years. Gastrointestinal disorders requiring dosage reduction or discontinuation of therapy, observed in five of nine patients, occurred at an incidence higher than expected from adult data. Our results suggest that the dose of 600 mg/m(2) every 12 h extrapolated from adult data for use in pediatric patients would be associated with plasma levels and AUCs higher than expected and may be associated with a higher incidence of side-effects, primarily gastrointestinal.
霉酚酸酯(MMF)是一种前体药物,可水解为活性免疫抑制剂霉酚酸(MPA)。该药物目前已广泛用于成年肾移植受者,其应用也已扩展到儿科患者,尽管该年龄组的药理学数据有限。9名儿科肾移植受者在移植后中位数55个月(范围7.5 - 124个月)接受了MMF联合皮质类固醇以及环孢素或他克莫司治疗。在以494±142 mg/m²的口服剂量每日两次给予MMF后,通过高效液相色谱法在稳态下测定MPA和MPA葡萄糖醛酸苷(MPAG)的药代动力学参数。MPA吸收迅速,在1.4小时达到峰值浓度。稳态下MPA的平均血浆浓度为4.7±1.3μg/ml。在12小时(两次给药之间)血浆浓度 - 时间曲线(AUC)下的面积,MPA为57.0±15.3μg·h/ml,MPAG为1515±722μg·h/ml,MPA和MPAG的表观口服清除率分别为11.7±7.9和0.5±0.4 l/h。假设MPA的药代动力学呈剂量依赖性,针对每12小时600 mg/m²的推荐给药方案计算了MPA的稳态平均浓度和AUC分别为6.3±2.7μg/ml和75.2±32.9μg·h/ml。对MMF的耐受性进行了前瞻性研究,随访时间为1.1±年。9名患者中有5名出现需要减少剂量或停药的胃肠道疾病,其发生率高于成人数据预期。我们的结果表明,从成人数据外推用于儿科患者的每12小时600 mg/m²剂量可能会导致血浆水平和AUC高于预期,并可能伴有更高的副作用发生率,主要是胃肠道副作用。
