供体肾的潜伏性IgA沉积是肾移植中复发性IgA肾病的主要危险因素。
Latent IgA deposition from donor kidney is the major risk factor for recurrent IgA nephropathy in renal transplantation.
作者信息
Moriyama Takahito, Nitta Kosaku, Suzuki Koichi, Honda Kazuho, Horita Shigeru, Uchida Keiko, Yumura Wako, Tanabe Kazunari, Toma Hiroshi, Nihei Hiroshi, Yamaguchi Yutaka
机构信息
Department of Medicine, Kidney Center, Tokyo Women's Medical University, Tokyo, Japan.
出版信息
Clin Transplant. 2005;19 Suppl 14:41-8. doi: 10.1111/j.1399-0012.2005.00403.x.
BACKGROUND
Previous studies have recognized risk factors for recurrent IgA nephropathy (r-IgAN) in renal transplantation. However the clinical significance of latent IgA deposition from the donor kidney remains to be determined.
PATIENTS AND METHODS
Between 1992 and 1999, 0-hour allograft biopsies were performed in 510 renal transplantation recipients at the Kidney Center of Tokyo Women's Medical University. Among these 510 patients, there were 49 whose primary disease was identified as IgAN. Among these 49 patients, 13 patients (26.5%) were diagnosed as having r-IgAN based on renal biopsy. We compared risk factors of r-IgAN, including IgA deposition, between the r-IgAN and non-r-IgAN groups.
RESULTS
We assessed factors previously reported to be risk factors for r-IgAN, such as follow-up period after transplantation, sex, ages of donors and recipients, donor type, ABO compatible or incompatible transplantation, number of HLA-A, B, and DR mismatches, number of donors with HLA-A2, B35, B46, and/or DR4, duration to end stage renal disease, duration of dialysis, and latent IgA deposition from donor kidneys. Latent IgA deposition was the only risk factor that differed significantly in frequency between patients with and without recurrence (38.5% in r-IgAN group vs. 9.1% in non-r-IgAN group, p = 0.037). Other factors did not differ significantly between the two groups. Clinical factors, such as urinary protein excretion, urinary red blood cell sediment and serum creatinine, were significantly worse and the number of patients who required hemodialysis 5 yr after transplantation was significantly higher in the r-IgAN group than in the non-r-IgAN group (38.5 vs. 5.6%, p = 0.001). Four of the five patients who required hemodialysis in the r-IgAN group had latent IgA deposition from the donor kidney.
CONCLUSION
Our data suggest that 26.5% out of patients with primary IgAN will develop recurrence within 5 yr after transplantation. Latent IgA deposition from the donor kidney was one of the risk factors of r-IgAN and it would lead to the development of r-IgAN. Moreover, r-IgAN will compromise graft survival, especially in cases with latent IgA deposition from the donor kidney.
背景
既往研究已明确肾移植中复发性IgA肾病(r-IgAN)的危险因素。然而,供肾中潜在IgA沉积的临床意义仍有待确定。
患者与方法
1992年至1999年间,东京女子医科大学肾脏中心对510例肾移植受者进行了移植肾0小时活检。在这510例患者中,有49例原发性疾病被诊断为IgA肾病。在这49例患者中,13例(26.5%)经肾活检诊断为r-IgAN。我们比较了r-IgAN组和非r-IgAN组r-IgAN的危险因素,包括IgA沉积情况。
结果
我们评估了先前报道的r-IgAN危险因素,如移植后的随访时间、性别、供受者年龄、供者类型、ABO血型相容或不相容移植、HLA-A、B和DR错配数、携带HLA-A2、B35、B46和/或DR4的供者数量、终末期肾病持续时间、透析时间以及供肾的潜在IgA沉积情况。潜在IgA沉积是复发患者与未复发患者之间频率差异有统计学意义的唯一危险因素(r-IgAN组为38.5%,非r-IgAN组为9.1%,p = 0.037)。两组间其他因素差异无统计学意义。r-IgAN组的临床指标,如尿蛋白排泄、尿红细胞沉降率和血清肌酐,明显更差,且移植后5年需要血液透析的患者数量显著高于非r-IgAN组(38.5%对5.6%,p = 0.001)。r-IgAN组需要血液透析的5例患者中有4例存在供肾潜在IgA沉积。
结论
我们的数据表明,原发性IgA肾病患者中有26.5%会在移植后5年内复发。供肾潜在IgA沉积是r-IgAN的危险因素之一,会导致r-IgAN的发生。此外,r-IgAN会影响移植肾存活,尤其是在存在供肾潜在IgA沉积的情况下。
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