Transplantation. 1999 Aug 15;68(3):391-6.
The European double-blind, placebo(PLA) controlled study of mycophenolate mofetil (MMF) for prevention of acute renal allograft rejection showed that MMF 2 and 3 g when added to a standard double-drug regimen of cyclosporine and corticosteroids significantly reduced the incidence of acute rejection/treatment failure at 6 months. Our study presents 3-year data for patient and graft survival, and safety in the MMF-treated patients.
The trial included 491 patients who were randomly assigned to receive PLA (n=166), MMF 2g (n=165), or MMF 3 g (n=160). Patients in the PLA group discontinued taking their PLA medication at 1 year posttransplantation; subsequently, they were followed-up only regarding patient and graft survival and the occurrence of malignancies.
The 3-year patient survival was 88.9, 92.7, and 91.8% in the PLA, MMF 2 g, and MMF 3 g groups, respectively. The 3-year graft survival (including death as a cause of graft loss) was 78, 84.8, and 81.2%, respectively. Acute allograft rejection was a principal cause of graft loss in all groups (PLA, 10.8%; MMF 2 g, 4.6%; MMF 3 g, 6.3%). Differences in 3-year graft loss rates (excluding death) and 95% confidence intervals for intent-to-treat comparisons of PLA versus MMF 2 g and 3 g, respectively, were 7.3% (1.1, 14.2) and 3.2% (-3.8, 10.1). This leads to a relative risk of graft loss of 0.55 in the MMF 2 g arm compared with the PLA arm. Acute allograft rejection had a major impact on graft loss at 3 years; 31.5% of patients with biopsy-proven acute rejection within 6 months of transplantation lost their graft by the end of 3 years. In contrast, only 6.6% who had no early acute rejection lost their graft by the end of the 3-year study period. Diarrhea, anemia, and leukopenia were the most common clinically relevant adverse events, occurring predominantly in the MMF 3 g group. Only one patient (MMF 3 g) developed cytomegalovirus tissue-invasive disease after the first year posttransplant. Over the 3-year posttransplant period, 12 patients developed malignancies (5 in the PLA group, 3 in the MMF 2 g group, and 4 in the MMF 3 g group).
At 3 years posttransplantation, MMF was associated with 7.6% reduction in the incidence of graft loss (excluding death). These data indicate that MMF treatment not only results in a reduction of the incidence of acute rejections but also leads to reduction of late allograft loss.
欧洲一项关于霉酚酸酯(MMF)预防肾移植急性排斥反应的双盲、安慰剂(PLA)对照研究表明,在环孢素和皮质类固醇标准双药方案基础上加用2克和3克MMF可显著降低6个月时急性排斥反应/治疗失败的发生率。我们的研究展示了MMF治疗患者3年的患者和移植物存活率及安全性数据。
该试验纳入491例患者,随机分配接受PLA(n = 166)、2克MMF(n = 165)或3克MMF(n = 160)治疗。PLA组患者在移植后1年停用PLA药物;随后,仅对患者和移植物存活率及恶性肿瘤发生情况进行随访。
PLA组、2克MMF组和3克MMF组的3年患者存活率分别为88.9%、92.7%和91.8%。3年移植物存活率(包括因移植物丢失导致的死亡)分别为78%、84.8%和81.2%。急性移植物排斥是所有组移植物丢失的主要原因(PLA组为10.8%;2克MMF组为4.6%;3克MMF组为6.3%)。PLA分别与2克MMF和3克MMF意向性治疗比较的3年移植物丢失率(不包括死亡)差异及95%置信区间分别为7.3%(1.1,14.2)和3.2%(-3.8,10.1)。这导致2克MMF组与PLA组相比移植物丢失的相对风险为0.55。急性移植物排斥对3年时的移植物丢失有重大影响;移植后6个月内经活检证实有急性排斥反应的患者中,31.5%在3年结束时失去移植物。相比之下,在3年研究期结束时,无早期急性排斥反应的患者中只有6.6%失去移植物。腹泻、贫血和白细胞减少是最常见的临床相关不良事件,主要发生在3克MMF组。移植后第1年之后,只有1例患者(3克MMF组)发生巨细胞病毒组织侵袭性疾病。在移植后的3年期间,12例患者发生恶性肿瘤(PLA组5例,2克MMF组3例,3克MMF组4例)。
移植后3年,MMF使移植物丢失发生率(不包括死亡)降低了7.6%。这些数据表明,MMF治疗不仅可降低急性排斥反应的发生率,还可减少晚期移植物丢失。
