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mTOR Inhibition and Clinical Transplantation: Liver

机译:mTOR抑制和临床移植:肝脏

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摘要

The evidence base concerning use of mammalian target of rapamycin (mTOR) inhibitor therapy after liver transplantation is evolving rapidly, clarifying their benefits and disadvantages in different clinical scenarios. The H2304 trial showed that starting everolimus at 1month posttransplant, with reduced tacrolimus, achieves a sustained improvement in renal function versus standard tacrolimus-based therapy, with at least equivalent immunosuppressive efficacy. Randomized studies evaluating early discontinuation of calcineurin inhibitor (CNI) therapy after introduction of an mTOR inhibitor consistently demonstrated a substantial improvement in renal function versus standard CNI therapy. However, concomitant mycophenolic acid is advisable to avoid an increase in mild biopsy-proven acute rejection, and induction with an interleukin-2 receptor antagonist may also be helpful. High-quality robust data regarding prevention of posttransplant malignancies under mTOR inhibitors is lacking in liver transplantation, although there are some indications of benefit. In maintenance patients, robust data are limited regarding mTOR inhibitor initiation in response to deteriorating renal function or other indications but late conversion ( 1 year) appears ineffective. Rates of mTOR inhibitor discontinuation due to adverse events are high, affecting at least a quarter of patients. In conclusion, the evidence base for use of mTOR inhibitors early posttransplant to support CNI reduction now convincingly demonstrates a renal advantage, but adequate adjunctive immunosuppression is essential to preserve efficacy.
机译:关于肝移植术后使用哺乳动物抑制剂治疗哺乳动物靶标的证据基础正在快速发展,阐明其在不同临床情景中的益处和缺点。 H2304试验表明,在1个月后血管血症,具有减少的Tacolimus,患有肾功能与标准巨杆菌的治疗的持续改善,至少等同的免疫抑制效果。在引入MTOR抑制剂后,评估钙调抑制剂早期停药(CNI)治疗的随机研究始终如一地证明了肾功能与标准CNI治疗的显着提高。然而,伴随的霉酚酸是建议避免轻度活组织检查成熟的急性排斥反应的增加,并且白细胞介素-2受体拮抗剂的诱导也可能有所帮助。关于预防MTOR抑制剂的预防患者恶性肿瘤的高质量稳健数据缺乏肝移植,尽管有一些益处的迹象。在维护患者中,有限于MTOR抑制剂的启动有限响应肾功能或其他适应症,但是晚期转化(& 1年)似乎无效。由于不良事件导致的MTOR抑制剂停止的速率很高,影响至少四分之一的患者。总之,使用MTOR抑制剂的证据基础,早期的后移植物支持CNI还原的令人信服地证明了肾脏优势,但足够的辅助免疫抑制对于保持功效至关重要。

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