[儿童肾移植和活体供体——因其必要性而无价]。

E Leumann, P Goetschel, T J Neuhaus, P M Ambühl, D Candinas
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引用次数: 0

摘要

未标记:肾移植是终末期肾衰竭患儿的首选治疗方法。由于尸体供体短缺和等待时间越来越长,活体供体移植(LDT)已成为一种重要的治疗选择。方法:1992年至1999年间,苏黎世共有48例儿童和青少年患者接受了肾移植。其中,21名患者(44%)接受了来自活体亲属供体的肾脏。11例患者在LDT前透析0.2-5.7年(中位0.6年),10例患者提前移植。三重免疫抑制包括环孢素A、硫唑嘌呤或霉酚酸酯(MMF);自1998年以来)和强的松。观察时间0.5 ~ 7.3年(中位2年)。结果:移植时受者年龄2 ~ 18岁(中位10.5岁)。三分之一的人患有先天性畸形、遗传性疾病或后天疾病。1例患者在移植后4个月死于相关心脏病,1例移植后2.8年发生功能丧失。9例患者从环孢素转为他克莫司,7例为活检证实的排斥反应,2例为美容原因(多毛症)。未使用抗体制剂。11名供体/受体一年后测量的中位肾小球滤过率(51Cr-EDTA)分别为64(55-95)和54 (32-82)ml/min/1.73 m2。19例功能性移植物的最新估计肾功能(Schwartz公式)为37-79 ml/min/1.73 m2(中位数63)。16例无相关肾外疾病患者的中位身高为-0.9 SDS(标准差评分);其余3名患有严重的肾外疾病,发育严重迟缓。主要并发症为可逆性排斥反应19例(90%),动脉高血压16例,巨细胞病毒病2例,无症状巨细胞病毒感染3例,肾盂肾炎3例,原发肾病复发、癫痫发作、糖尿病和不依从性各1例。3年后精算患者和移植物存活率(Kaplan-Meier)分别为95%和83%。这与尸体供体组(n = 27)的存活率(分别为100%和80%)没有统计学差异。整体康复情况良好。捐赠者为12位母亲、8位父亲和1位祖母,年龄31 ~ 50岁(中位39岁);他们都没有出现严重的术后问题。结论:在瑞士,如果没有LDT,儿科移植计划将不再可行。结果非常令人鼓舞;先发制人的移植使一半的患者可以避免透析。捐赠者的风险很小,在不给家庭施加压力的情况下进行仔细评估是至关重要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Pediatric kidney transplantation and living donors--invaluable by virtue of necessity].

Unlabelled: Renal transplantation is the treatment of choice for paediatric patients with end-stage renal failure. Living donor transplantation (LDT) has become an important therapeutic option due to the shortage of cadaver donors and increasingly long waiting times.

Methods: Between 1992 and 1999, a total of 48 paediatric and adolescent patients underwent renal transplantation in Zurich. Of these, 21 patients (44%) received a kidney from a living related donor. 11 patients had been dialysed before LDT over a period of 0.2-5.7 years (median 0.6), and 10 were transplanted preemptively. Triple immunosuppression consisted of cyclosporine A, azathioprine or mycophenolate mofetil (MMF; since 1998), and prednisone. The observation period was 0.5-7.3 years (median 2).

Results: Recipients were 2-18 (median 10.5) years old at transplantation. One third had either a congenital malformation, an inherited disease, or an acquired disorder. One patient died of an associated cardiac disease at 4 months with functioning graft, and one functional graft loss occurred after 2.8 years. 9 patients were switched from cyclosporine to tacrolimus, 7 for biopsy-proven rejection and 2 for cosmetic reasons (hypertrichosis). No antibody preparations were used. Median glomerular filtration rate (51Cr-EDTA), measured after one year in 11 donor/recipients, was 64 (55-95) and 54 (32-82) ml/min/1.73 m2, respectively. The most recent estimated renal function (Schwartz formula) of 19 functioning grafts was 37-79 ml/min/1.73 m2 (median 63). Median body height of 16 patients with no associated extrarenal disease was -0.9 SDS (standard deviation score); the remaining 3--with serious extra-renal disease--were considerably growth retarded. Main complications were reversible rejection episodes in 19 (90%), arterial hypertension (16), CMV disease (2) and asymptomatic CMV infection (3), pyelonephritis (3), and recurrence of the primary renal disease, seizures, diabetes mellitus and non-compliance (one each). Actuarial patient and graft survival (Kaplan-Meier) after 3 years was 95 and 83% respectively. This was not statistically different from the cadaveric donor group (n = 27) with 100 and 80% survival respectively. Overall rehabilitation was excellent. The donors were 12 mothers, 8 fathers and one grandmother aged 31 to 50 (median 39) years; none of them experienced serious postoperative problems.

Conclusions: The paediatric transplantation programme would no longer be feasible in Switzerland without LDT. The results are very encouraging; preemptive transplantation makes it possible to avoid dialysis in half of the patients. The risk for the donor is small, and careful evaluation without putting pressure on the family is essential.

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