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Transcriptome Analysis in Renal Transplant Biopsies Not Fulfilling Rejection Criteria

机译:肾移植活组织检查的转录组分析不满足排斥标准

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The clinical significance of renal transplant biopsies displaying borderline changes suspicious for T-cell mediated rejection (TCMR) or interstitial fibrosis and tubular atrophy (IFTA) with interstitial inflammation has not been well defined. Molecular profiling to evaluate renal transplant biopsies using microarrays has been shown to be an objective measurement that adds precision to conventional histology. We review the contribution of transcriptomic analysis in surveillance and indication biopsies with borderline changes and IFTA associated with variable degrees of inflammation. Transcriptome analysis applied to biopsies with borderline changes allows to distinguish patients with rejection from those in whom mild inflammation mainly represents a response to injury. Biopsies with IFTA and inflammation occurring in unscarred tissue display a molecular pattern similar to TCMR while biopsies with IFTA and inflammation in scarred tissue, apart from T-cell activation, also express B cell, immunoglobulin and mast cell-related genes. Additionally, patients at risk for IFTA progression can be identified by genes mainly reflecting fibroblast dysregulation and immune activation. At present, it is not well established whether the expression of rejection gene transcripts in patients with fibrosis and inflammation is the consequence of an alloimmune response, tissue damage or a combination of both.
机译:肾移植活组织检查显示临床意义显示濒临介导的T细胞介导的抑制(TCMR)或间质纤维化和管状萎缩(IFTA)没有明确定义。用于评估使用微阵列的肾移植活组织检查的分子分析已被证明是对常规组织学增加精度的客观测量。我们审查了转发组分析在具有临界变化和IFTA与可变性炎症相关的IFTA的临床和指示活组织检查的贡献。应用于具有边缘变化的活组织检查的转录组分析允许将患者区分为抑制症,其中炎症主要代表对损伤的反应。在未阵列组织中发生的IFTA和炎症的活组织检查显示了类似于TCMR的分子模式,同时具有IFTA的活组织检查和瘢痕组织中的炎症,除了T细胞活化,还表达B细胞,免疫球蛋白和肥大细胞相关基因。另外,IFTA进展的风险患者可以通过主要反映成纤维细胞失调和免疫活化的基因鉴定。目前,纤维化和炎症患者的抑制基因转录物的表达是不明确的,这是同种异性反应,组织损伤或两者组合的结果。

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