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A molecular classifier for predicting future graft loss in late kidney transplant biopsies

机译:用于预测晚期肾移植活检中未来移植物丢失的分子分类器

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摘要

Kidney transplant recipients that develop signs of renal dysfunction or proteinuria one or more years after transplantation are at considerable risk for progression to renal failure. To assess the kidney at this time, a “for-cause” biopsy is performed, but this provides little indication as to which recipients will go on to organ failure. In an attempt to identify molecules that could provide this information, we used micorarrays to analyze gene expression in 105 for-cause biopsies taken between 1 and 31 years after transplantation. Using supervised principal components analysis, we derived a molecular classifier to predict graft loss. The genes associated with graft failure were related to tissue injury, epithelial dedifferentiation, matrix remodeling, and TGF-β effects and showed little overlap with rejection-associated genes. We assigned a prognostic molecular risk score to each patient, identifying those at high or low risk for graft loss. The molecular risk score was correlated with interstitial fibrosis, tubular atrophy, tubulitis, interstitial inflammation, proteinuria, and glomerular filtration rate. In multivariate analysis, molecular risk score, peritubular capillary basement membrane multilayering, arteriolar hyalinosis, and proteinuria were independent predictors of graft loss. In an independent validation set, the molecular risk score was the only predictor of graft loss. Thus, the molecular risk score reflects active injury and is superior to either scarring or function in predicting graft failure.
机译:移植后一年或一年以上出现肾功能不全或蛋白尿迹象的肾移植受者有发展为肾衰竭的巨大风险。为了在此时评估肾脏,进行了“因果”活检,但这几乎没有迹象表明哪些接受者会继续器官衰竭。为了鉴定可提供此信息的分子,我们使用微阵列分析了在移植后1至31年间进行的105例活检组织中的基因表达。使用监督的主成分分析,我们得出了一个分子分类器来预测移植物的损失。与移植失败相关的基因与组织损伤,上皮去分化,基质重塑和TGF-β效应有关,与排斥相关基因几乎没有重叠。我们为每位患者分配了预后分子风险评分,以识别出移植物丢失风险高或低的患者。分子风险评分与间质纤维化,肾小管萎缩,肾小管炎,间质性炎症,蛋白尿和肾小球滤过率相关。在多变量分析中,分子风险评分,肾小管毛细血管基底膜多层性,小动脉透明质酸和蛋白尿是移植物丢失的独立预测因素。在独立的验证集中,分子风险评分是移植物损失的唯一预测因子​​。因此,分子风险评分反映了活动性损伤,并且在瘢痕形成或预测移植失败方面的作用均优于瘢痕形成或功能。

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