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肝移植受者维持期从钙调神经磷酸酶抑制剂转换为依维莫司治疗:一项前瞻性、随机、多中心试验。

Conversion from a calcineurin inhibitor to everolimus therapy in maintenance liver transplant recipients: a prospective, randomized, multicenter trial.

作者信息

De Simone Paolo, Metselaar Herold J, Fischer Lutz, Dumortier Jérôme, Boudjema Karim, Hardwigsen Jean, Rostaing Lionel, De Carlis Luciano, Saliba Faouzi, Nevens Frederik

机构信息

Liver Transplantation Department, Azienda Ospedaliero-Universitaria Pisana, Pisa, Italy.

出版信息

Liver Transpl. 2009 Oct;15(10):1262-9. doi: 10.1002/lt.21827.

DOI:10.1002/lt.21827
PMID:19790150
Abstract

Calcineurin inhibitors (CNIs) contribute to renal dysfunction following liver transplantation. This prospective, randomized, multicenter, 6-month study (with an additional 6 months of follow-up) evaluated whether everolimus with CNI reduction or discontinuation would improve renal function in maintenance liver transplant recipients experiencing CNI-related renal impairment. Patients started everolimus therapy with CNI reduction or discontinuation (n = 72) or continued receiving standard-exposure CNI (n = 73). At month 6, 80% of the patients who had converted to everolimus had discontinued the CNI. The mean change in creatinine clearance (CrCl) from baseline to month 6 was similar between groups (everolimus, 1.0 +/- 10.2 mL/minute; controls, 2.3 +/- 7.8 mL/minute; P = 0.46), so the primary study endpoint (8 mL/minute difference in the change in CrCl) was not achieved. Among patients who continued everolimus according to the protocol, the mean increase in CrCl was 2.1 (n = 53) and 3.8 mL/minute (n = 38) at months 6 and 12, respectively, versus 2.4 (n = 68) and 3.5 mL/minute in controls (n = 51). The high frequency of CNI dose reductions in controls (77% of the patients) and the relatively long mean time post-transplant (>3 years) likely contributed to the small difference in CrCl. Biopsy-proven acute rejection occurred in 1.4% of the patients in each group, with no graft losses. Study drug discontinuation was higher in everolimus-treated patients, and adverse events were more frequent. These data demonstrate that everolimus allows for discontinuation or a major reduction of CNI exposure in liver allograft recipients suffering CNI-related renal dysfunction without a loss of efficacy. Trials targeting earlier conversion post-transplantation are required to confirm the efficacy and safety of everolimus for improving renal function after liver transplantation.

摘要

钙调神经磷酸酶抑制剂(CNIs)会导致肝移植后出现肾功能障碍。这项前瞻性、随机、多中心、为期6个月的研究(另有6个月的随访期)评估了在经历CNI相关肾功能损害的肝移植受者中,使用依维莫司并减少或停用CNI是否能改善肾功能。患者开始接受依维莫司治疗并减少或停用CNI(n = 72),或继续接受标准剂量的CNI(n = 73)。在第6个月时,转换为依维莫司治疗的患者中有80%已停用CNI。两组从基线到第6个月时肌酐清除率(CrCl)的平均变化相似(依维莫司组,1.0±10.2 mL/分钟;对照组,2.3±7.8 mL/分钟;P = 0.46),因此未达到主要研究终点(CrCl变化差值为8 mL/分钟)。在按照方案继续使用依维莫司的患者中,第6个月和第12个月时CrCl的平均增加量分别为2.1(n = 53)和3.8 mL/分钟(n = 38),而对照组分别为2.4(n = 68)和3.5 mL/分钟(n = 51)。对照组中CNI剂量减少的频率较高(77%的患者)以及移植后平均时间相对较长(>3年)可能导致了CrCl的差异较小。每组中1.4%的患者发生了活检证实的急性排斥反应,且无移植物丢失。依维莫司治疗的患者中研究药物停药率较高,不良事件也更频繁。这些数据表明,依维莫司可使患有CNI相关肾功能障碍的肝移植受者停用CNI或大幅减少CNI暴露,且不损失疗效。需要针对移植后更早转换治疗的试验来确认依维莫司改善肝移植后肾功能的有效性和安全性。

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