首页> 外文期刊>Journal of nephrology. >Kidney transplant in patients with atypical hemolytic uremic syndrome in the anti-C5 era: single-center experience with tailored Eculizumab
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Kidney transplant in patients with atypical hemolytic uremic syndrome in the anti-C5 era: single-center experience with tailored Eculizumab

机译:抗 C5 时代非典型溶血性尿毒症综合征患者的肾移植:定制依库珠单抗的单中心经验

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Rationale and objective Patients with atypical hemolytic uremic syndrome (aHUS) have long been considered ineligible for kidney transplantation (KTx) in several centers due to the high risk of disease recurrence, graft loss and life-threatening complications. The availability of Eculizumab (ECU) has now overcome this problem. However, the best approach towards timing, maintenance schedule, the possibility of discontinuation and patient monitoring has not yet been clearly established. Study design This is a single center case series presenting our experience with KTx in aHUS. Setting and participants This study included 26 patients (16 females) with a diagnosis of aHUS, who spent a median of 5.5 years on kidney replacement therapy before undergoing KTx. We compared the aHUS relapse rate in three groups of patients who underwent KTx: patients who received no prophylaxis, patients who underwent plasma exchange, those who received Eculizumab prophylaxis. Complement factor H-related disease was by far the most frequent etiology (n = 19 patients). Results Untreated patients and patients undergoing pre-KTx plasma exchange prophylaxis had a relapse rate of 0.81 (CI 0.30-1.76) and 3.1 (CI 0.64-9.16) events per 10 years cumulative observation, respectively, as opposed to 0 events among patients receiving Eculizumab prophylaxis. The time between Eculizumab doses was tailored based on classic complement pathway activity (target to < 30). Using this strategy, 12 patients are currently receiving Eculizumab every 28 days, 5 every 24-25 days, and 3 every 21 days. Conclusion Our experience supports the prophylactic use of Eculizumab in patients with a previous history of aHUS undergoing KTx, especially when complement dysregulation is well documented by molecular biology. Graphic abstract
机译:基本原理和目的 非典型溶血性尿毒症综合征 (aHUS) 患者长期以来被认为不适合肾移植 (KTx),因为疾病复发、移植物丢失和危及生命的并发症风险很高。依库珠单抗(ECU)的上市现在已经克服了这个问题。然而,时机、维持计划、停药可能性和患者监测的最佳方法尚未明确确定。研究设计 这是一个单一中心病例系列,展示了我们在 aHUS 中使用 KTx 的经验。环境和参与者 这项研究包括 26 名诊断为 aHUS 的患者(16 名女性),他们在接受 KTx 之前接受肾脏替代治疗的中位时间为 5.5 年。我们比较了接受KTx的三组患者的aHUS复发率:未接受预防的患者、接受血浆置换的患者、接受依库珠单抗预防的患者。补体因子 H 相关疾病是迄今为止最常见的病因(n = 19 例患者)。结果 未经治疗的患者和接受KTx前血浆置换预防的患者每10年累积观察的复发率分别为0.81(CI 0.30-1.76)和3.1(CI 0.64-9.16),而接受依库珠单抗预防治疗的患者为0。依库珠单抗剂量之间的时间是根据经典补体途径活性(目标< 30%)定制的。使用这种策略,目前有 12 名患者每 28 天接受一次 Eculizumab,每 24-25 天接受 5 名患者,每 21 天接受 3 名患者。结论 我们的经验支持在既往有 aHUS 病史且接受 KTx 的患者中预防性使用 Eculizumab,尤其是当分子生物学充分证明补体失调时。图形摘要

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