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Recurrent IgA nephropathy in renal transplant allografts.

机译:移植肾移植物中复发性IgA肾病。

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Previous reports of renal transplantation for patients with underlying immunoglobulin A (IgA) nephropathy suggested a recurrence rate greater than 50% for transplant IgA nephropathy. Initially regarded as a benign condition, more recent data showed that recurrent transplant IgA nephropathy may be a significant contributor to graft loss. We performed a retrospective analysis in a single center of 48 kidney transplant recipients, all of Chinese origin, with biopsy-proven IgA nephropathy as the cause of end-stage renal failure to determine the recurrence rate of IgA nephropathy in the transplant allograft and subsequent clinical course in Chinese patients. Median duration of follow-up was 52 months (range, 18 to 155 months). Fourteen patients (29%) had biopsy-confirmed recurrent transplant IgA nephropathy after a median of 52 months (interquartile range, 23 to 82 months) posttransplantation. Recurrent transplant IgA nephropathy was associated with greater serum IgA levels (P = 0.01). The presence of HLA-A2 in transplant recipients (P = 0.002) appeared to protect them from developing recurrent IgA nephropathy in the transplant allograft. Twenty-nine percent of patients with recurrent transplant IgA nephropathy had progressive deterioration of graft function. The progressive graft dysfunction (GD) rate was greater in patients with a transplant from a living related donor (LRD; 21%) compared with those with a transplant from a cadaveric or living unrelated donor (URD; 3%; P = 0.062). Although the cumulative graft survival rate was 100% at 5 years for transplants from both LRDs and URDs, the 10-year graft survival rate was only 63% for a graft from an LRD versus 93% for a URD (log-rank test, P = 0.19). A review of other reported series of recurrent transplant IgA nephropathy also showed an apparently greater incidence of GD for a graft from an LRD (28%) compared with a URD (15%). Our data suggest that although recurrent transplant IgA nephropathy is highly prevalent among the Chinese population, the risk for disease recurrence is not particularly increased compared with other ethnic groups. The trend toward a greater risk for GD for living related compared with unrelated allografts in patients with IgA nephropathy needs to be confirmed with further prospective study.
机译:先前针对潜在免疫球蛋白A(IgA)肾病患者进行肾移植的报道表明,移植IgA肾病的复发率大于50%。最初被视为良性疾病,最近的数据表明,复发性移植IgA肾病可能是造成移植物丢失的重要原因。我们在48位来自中国的肾脏移植受者的单个中心进行了回顾性分析,以活检证实的IgA肾病为终末期肾衰竭的原因,以确定同种异体移植IgA肾病的复发率及后续临床中国患者的病程。中位随访时间为52个月(范围18到155个月)。移植后中位数为52个月(四分位间距为23至82个月),有14例患者(占29%)有活检证实为复发性移植IgA肾病。复发性移植IgA肾病与更高的血清IgA水平相关(P = 0.01)。移植受者中HLA-A2的存在(P = 0.002)似乎可以保护他们,使其免受移植同种异体中复发性IgA肾病的困扰。 29%的反复移植IgA肾病患者的移植物功能逐渐恶化。与从活体相关供体(LRD; 21%)进行移植的患者相比,从尸体或活体无关供体(URD; 3%; P = 0.062)进行移植的患者,进行性移植物功能障碍(GD)的发生率更高。尽管LRD和URD的移植物在5年时的累计移植存活率均为100%,但LRD移植物的10年移植物存活率仅为63%,而URD的移植物的10年移植物存活率仅为93%(对数秩检验,P = 0.19)。对其他报道的一系列复发性移植IgA肾病的综述也显示,与URD(15%)相比,LRD(28%)移植物的GD发生率明显更高。我们的数据表明,尽管复发性移植IgA肾病在中国人群中非常普遍,但与其他种族相比,疾病复发的风险并未特别增加。与不相关同种异体移植相比,IgA肾病患者的GD生存相关风险更高的趋势有待进一步的前瞻性研究证实。

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