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Introduction of everolimus in kidney transplant recipients at a late posttransplant stage

机译:移植后后期在肾脏移植受者中引入依维莫司

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摘要

This minireview focuses on the current knowledge about the introduction of everolimus (EVL), a mammalian target of rapamycin inhibitor, with calcineurin inhibitor (CNI) elimination or minimization in kidney transplant recipients at a late posttransplant stage. Within, we have summarized two major clinical trials, ASCERTAIN and APOLLO, and seven other retrospective or nonrandomized studies. In the open-label multicenter ASCERTAIN study, the estimated glomerular filtration rate (eGFR) at 24 mo after conversion was not significantly different between three groups-EVL with CNI elimination, CNI minimization and continued CNI unchanged-at a mean of 5.4 years after transplantation. However, recipients with baseline creatinine clearance higher than 50 mL/min had a greater increase in measured GFR after CNI elimination. In the open-label multicenter APOLLO study, adjusted eGFR within the on-treatment population was significantly higher in the EVL continuation group than in the CNI continuation group at 12 mo after conversion at a mean of 7 years posttransplantation. Other studies on recipients without adverse events and already having satisfactory renal function showed favorable graft function by EVL late-induction with CNI elimination or reduction. These studies showed that chronic allograft nephropathy, CNI nephrotoxicity, CNI arteriolopathy, cancer and viral infection (especially cytomegalovirus infection) may be good indications for late conversion to EVL.
机译:这份小型综述的重点是在移植后后期在肾移植受者中引入依维莫司(EVL)(雷帕霉素抑制剂的哺乳动物靶标)与钙调神经磷酸酶抑制剂(CNI)的消除或最小化有关的最新知识。其中,我们总结了两项主要的临床试验,即ASCERTAIN和APOLLO,以及其他七项回顾性或非随机性研究。在开放标签的多中心ASCERTAIN研究中,三组之间的转换后24个月时的估计肾小球滤过率(eGFR)在没有CNI消除,CNI最小化和持续CNI不变的EVL之间平均无差异-移植后平均5.4年。但是,基线肌酐清除率高于50 mL / min的接受者在CNI消除后的GFR测量值有较大增加。在开放标签的多中心APOLLO研究中,在移植后12个月(平均移植后7年),EVL持续治疗组中接受治疗的人群中调整后的eGFR显着高于CNI持续治疗组。其他对没有不良事件并且已经具有令人满意的肾功能的接受者的研究表明,通过EVL后期诱导和CNI消除或减少,移植者的功能良好。这些研究表明,慢性同种异体移植肾病,CNI肾毒性,CNI动脉病变,癌症和病毒感染(尤其是巨细胞病毒感染)可能是晚期转化为EVL的良好指征。

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