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肾移植受者尿液中平滑肌特异性肌动蛋白水平:与环孢素或他克莫司肾毒性的相关性。

Smooth muscle-specific actin levels in the urine of renal transplant recipients: correlation with cyclosporine or tacrolimus nephrotoxicity.

作者信息

Haas M, Meehan S M, Josephson M A, Wit E J, Woodle E S, Thistlethwaite J R

机构信息

Departments of Pathology and Statistics, University of Chicago, Chicago, IL, USA.

出版信息

Am J Kidney Dis. 1999 Jul;34(1):69-84. doi: 10.1016/s0272-6386(99)70111-3.

Abstract

Cyclosporine A (CSA) and tacrolimus (FK506) are powerful immunosuppressive agents that have proven useful for antirejection therapy in patients with solid organ transplants, including kidney. However, both drugs are nephrotoxic, each producing similar histological patterns of injury to renal tubules and preglomerular arterioles, and this toxicity is a major cause of renal allograft dysfunction. A renal transplant biopsy presently represents the most reliable means of diagnosing nephrotoxicity caused by CSA or tacrolimus and distinguishing it from acute rejection. Because CSA and tacrolimus nephrotoxicity often involve arteriolar smooth muscle, whereas vascular smooth muscle is rarely involved in acute rejection, we investigated if the appearance of a smooth muscle-specific isoform of alpha-actin (SMA) in the urine of renal transplant recipients about to undergo a biopsy for graft dysfunction correlated with biopsy evidence of CSA or tacrolimus toxicity. Eighty-nine urine samples from 61 patients, plus 6 samples from healthy control subjects, were analyzed in a blinded manner by enzyme-linked immunosorbent assay using a specific anti-SMA monoclonal antibody. For the patient samples, the results of these assays were then correlated with the biopsy findings. Those 40 cases in which the biopsy showed evidence of CSA or tacrolimus nephrotoxicity had a significantly (P < 0.01) greater SMA level in the corresponding urine samples (0.089 +/- 0.126 microgram/mL; mean +/- SD) than the 49 cases without toxicity (0.018 +/- 0.027 microgram/mL) or 6 control subjects (0.003 +/- 0.007 microgram/mL), although there was considerable overlap of SMA values among these groups. The greatest SMA levels were seen in patients with CSA or tacrolimus nephrotoxicity that was likely to be relatively acute, namely those with thrombotic microangiopathy and those without previous biopsy evidence of toxicity. SMA levels correlated significantly with the estimated severity of arteriolopathy on biopsy. In patients with tubular but not arteriolar lesions of CSA or tacrolimus toxicity, the mean SMA level was not significantly greater than that in patients without toxicity. Urine SMA levels in patients with a biopsy specimen showing acute rejection were not significantly different from those in patients without rejection, and there was no correlation between urine SMA level and severity of rejection. Whereas the degree of overlap of SMA levels in patients with and without nephrotoxicity was far too great to consider this assay as a potential alternative to renal transplant biopsy for the diagnosis of nephrotoxicity, the assay may have potential as a marker for active arteriolar injury in renal transplant recipients and other patients receiving CSA or tacrolimus therapy.

摘要

环孢素A(CSA)和他克莫司(FK506)是强效免疫抑制剂,已被证明对实体器官移植患者(包括肾移植患者)的抗排斥治疗有用。然而,这两种药物都具有肾毒性,各自产生相似的肾小管和肾小球前小动脉损伤组织学模式,并且这种毒性是肾移植功能障碍的主要原因。目前,肾移植活检是诊断CSA或他克莫司引起的肾毒性并将其与急性排斥反应区分开来的最可靠方法。由于CSA和他克莫司肾毒性常累及小动脉平滑肌,而血管平滑肌很少参与急性排斥反应,我们研究了即将因移植功能障碍接受活检的肾移植受者尿液中α-肌动蛋白(SMA)的平滑肌特异性同工型的出现是否与CSA或他克莫司毒性的活检证据相关。使用特异性抗SMA单克隆抗体,通过酶联免疫吸附测定法对61例患者的89份尿液样本以及6份健康对照者的样本进行了盲法分析。对于患者样本,然后将这些测定结果与活检结果相关联。活检显示有CSA或他克莫司肾毒性证据的40例患者,其相应尿液样本中的SMA水平(0.089±0.126微克/毫升;平均值±标准差)显著(P<0.01)高于49例无毒性患者(0.018±0.027微克/毫升)或6例对照者(0.003±0.007微克/毫升),尽管这些组之间的SMA值有相当大的重叠。在可能相对急性的CSA或他克莫司肾毒性患者中,即患有血栓性微血管病的患者和之前无活检毒性证据的患者中,观察到最高的SMA水平。SMA水平与活检时小动脉病变的估计严重程度显著相关。在有CSA或他克莫司毒性的肾小管而非小动脉病变的患者中,平均SMA水平并不显著高于无毒性患者。活检标本显示急性排斥反应的患者尿液SMA水平与无排斥反应患者的尿液SMA水平无显著差异,并且尿液SMA水平与排斥反应的严重程度之间无相关性。虽然有和没有肾毒性的患者之间SMA水平的重叠程度太大,以至于不能将该测定法视为肾移植活检诊断肾毒性的潜在替代方法,但该测定法可能有潜力作为肾移植受者和其他接受CSA或他克莫司治疗的患者活动性小动脉损伤的标志物。

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