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移植性肾小球病中基因表达的概率(贝叶斯)建模。

Probabilistic (Bayesian) modeling of gene expression in transplant glomerulopathy.

机构信息

Regenerative Medicine Department, Combat Casualty Care, Naval Medical Research Center, Silver Spring, Maryland 20910, USA.

出版信息

J Mol Diagn. 2010 Sep;12(5):653-63. doi: 10.2353/jmoldx.2010.090101. Epub 2010 Aug 5.

Abstract

Transplant glomerulopathy (TG) is associated with rapid decline in glomerular filtration rate and poor outcome. We used low-density arrays with a novel probabilistic analysis to characterize relationships between gene transcripts and the development of TG in allograft recipients. Retrospective review identified TG in 10.8% of 963 core biopsies from 166 patients; patients with stable function were studied for comparison. The biopsies were analyzed for expression of 87 genes related to immune function and fibrosis by using real-time PCR, and a Bayesian model was generated and validated to predict histopathology based on gene expression. A total of 57 individual genes were increased in TG compared with stable function biopsies (P < 0.05). The Bayesian analysis identified critical relationships between ICAM-1, IL-10, CCL3, CD86, VCAM-1, MMP-9, MMP-7, and LAMC2 and allograft pathology. Moreover, Bayesian models predicted TG when derived from either immune function (area under the curve [95% confidence interval] of 0.875 [0.675 to 0.999], P = 0.004) or fibrosis (area under the curve [95% confidence interval] of 0.859 [0.754 to 0.963], P < 0.001) gene networks. Critical pathways in the Bayesian models were also analyzed by using the Fisher exact test and had P values <0.005. This study demonstrates that evaluating quantitative gene expression profiles with Bayesian modeling can identify significant transcriptional associations that have the potential to support the diagnostic capability of allograft histology. This integrated approach has broad implications in the field of transplant diagnostics.

摘要

移植肾小球病(TG)与肾小球滤过率的快速下降和不良预后有关。我们使用具有新型概率分析的低密度阵列来描述基因转录物与同种异体移植物受者 TG 发展之间的关系。回顾性研究在 166 名患者的 963 例核心活检中发现 10.8%的 TG;为了比较,研究了功能稳定的患者。通过实时 PCR 分析活检中与免疫功能和纤维化相关的 87 个基因的表达,并生成和验证贝叶斯模型,根据基因表达预测组织病理学。与功能稳定的活检相比,TG 中共有 57 个单独的基因增加(P <0.05)。贝叶斯分析确定了 ICAM-1、IL-10、CCL3、CD86、VCAM-1、MMP-9、MMP-7 和 LAMC2 与同种异体移植物病理之间的关键关系。此外,当从免疫功能(曲线下面积[95%置信区间]为 0.875 [0.675 至 0.999],P = 0.004)或纤维化(曲线下面积[95%置信区间]为 0.859 [0.754 至 0.963],P <0.001)基因网络得出贝叶斯模型时,也可以预测 TG。还通过 Fisher 精确检验分析了贝叶斯模型中的关键途径,其 P 值 <0.005。这项研究表明,使用贝叶斯建模评估定量基因表达谱可以识别具有支持同种异体组织学诊断能力的重要转录关联。这种综合方法在移植诊断领域具有广泛的意义。

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