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肾移植受者转换为西罗莫司治疗后的蛋白尿。

Proteinuria after conversion to sirolimus in renal transplant recipients.

作者信息

Sahin G M, Sahin S, Kantarci G, Ergin H

机构信息

Department of Nephrology, Goztepe Research and Teaching Hospital, Istanbul, Turkey.

出版信息

Transplant Proc. 2006 Dec;38(10):3473-5. doi: 10.1016/j.transproceed.2006.10.152.

Abstract

Sirolimus (SRL) is a new, potent immunosuppressive agent. More recently, proteinuria has been reported as a consequence of sirolimus therapy, although the mechanism has remained unclear. We retrospectively examined the records of 25 renal transplant patients, who developed or displayed increased proteinuria after SRL conversion. The patient cohort (14 men, 11 women) was treated with SRL as conversion therapy, due to chronic allograft nephropathy (CAN) (n = 15) neoplasia (n = 8); Kaposi's sarcoma, Four skin cancers, One intestinal tumors, One renal cell carsinom) or BK virus nephropathy (n = 2). SRL was started at a mean of 78 +/- 42 (15 to 163) months after transplantation. Mean follow-up on SRL therapy was 20 +/- 12 (6 to 43) months. Proteinuria increased from 0.445 (0 to 1.5) g/d before conversion to 3.2 g/dL (0.2 to 12) after conversion (P = 0.001). Before conversion 8 (32%) patients had no proteinuria, whereas afterwards all patients had proteinuria. In 28% of patients proteinuria remained unchanged, whereas it increased in 68% of patients. In 40% it increased by more than 100%. Twenty-eight percent of patients showed increased proteinuria to the nephrotic range. Biopsies performed in five patients revealed new pathological changes: One membranoproliferative glomerulopathy and interstitial nephritis. These patients showed persistently good graft function. Serum creatinine values did not change significantly: 1.98 +/- 0.8 mg/dL before SRL therapy and 2.53 +/- 1.9 mg/dL at last follow-up (P = .14). Five grafts were lost and the patients returned to dialysis. Five patients displayed CAN and Kaposi's sarcoma. Mean urinary protein of patients who returned to dialysis was 1.26 (0.5 to 3.5) g/d before and 4.7 (3 to 12) g/d after conversion (P = .01). Mean serum creatinine level before conversion was 2.21 mg/dL and thereafter, 4.93 mg/dL (P = .02). Heavy proteinuria was common after the use of SRL as rescue therapy for renal transplantation. Therefore, conversion should be considered for patients who have not developed advanced CAN and proteinuria. The possibility of de novo glomerular pathology under SRL treatment requires further investigation by renal biopsy.

摘要

西罗莫司(SRL)是一种新型强效免疫抑制剂。最近,有报道称西罗莫司治疗会导致蛋白尿,但其机制尚不清楚。我们回顾性研究了25例肾移植患者的记录,这些患者在转换使用西罗莫司后出现蛋白尿或蛋白尿增加。患者队列包括14名男性和11名女性,因慢性移植肾肾病(CAN)(n = 15)、肿瘤(n = 8);卡波西肉瘤、4例皮肤癌、1例肠道肿瘤、1例肾细胞癌或BK病毒肾病(n = 2)接受西罗莫司作为转换治疗。西罗莫司在移植后平均78±42(15至163)个月开始使用。西罗莫司治疗的平均随访时间为20±12(6至43)个月。蛋白尿从转换前的0.445(0至1.5)g/d增加到转换后的3.2 g/dL(0.2至12)(P = 0.001)。转换前8例(32%)患者无蛋白尿,而转换后所有患者均出现蛋白尿。28%的患者蛋白尿保持不变,而68%的患者蛋白尿增加。40%的患者蛋白尿增加超过100%。28%的患者蛋白尿增加至肾病范围。对5例患者进行的活检显示有新的病理变化:1例膜增生性肾小球病和间质性肾炎。这些患者的移植肾功能持续良好。血清肌酐值无显著变化:西罗莫司治疗前为1.98±0.8 mg/dL,最后一次随访时为2.53±1.9 mg/dL(P = 0.14)。5例移植肾失功,患者重新开始透析。5例患者患有CAN和卡波西肉瘤。重新开始透析的患者转换前平均尿蛋白为1.26(0.5至3.5)g/d,转换后为4.7(3至12)g/d(P = 0.01)。转换前平均血清肌酐水平为2.21 mg/dL,之后为4.93 mg/dL(P = 0.02)。使用西罗莫司作为肾移植挽救治疗后,重度蛋白尿很常见。因此,对于尚未发生晚期CAN和蛋白尿的患者应考虑进行转换。西罗莫司治疗下出现新发肾小球病变的可能性需要通过肾活检进一步研究。

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