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在急性肾移植排斥反应早期的外周血中进行功能基因组分析。

Functional genomic analysis of peripheral blood during early acute renal allograft rejection.

机构信息

PROOF Centre of Excellence, University of British Columbia, Vancouver, BC V5Z 1M9, Canada.

出版信息

Transplantation. 2009 Oct 15;88(7):942-51. doi: 10.1097/TP.0b013e3181b7ccc6.

Abstract

BACKGROUND

Acute graft rejection is an important clinical problem in renal transplantation and an adverse predictor for long-term graft survival. Peripheral blood biomarkers that provide evidence of early graft rejection may offer an important option for posttransplant monitoring, optimize the utility of graft biopsy, and permit timely and effective therapeutic intervention to minimize the graft damage.

METHODS

In this feasibility study (n=58), we have used gene expression profiling in a case-control design to compare whole blood samples between normal subjects (n=20) and patients with (n=11) or without (n=22) biopsy-confirmed acute rejection (BCAR) or borderline changes (n=5).

RESULTS

A total of 183 probe sets representing 160 genes were differentially expressed (false discovery rate [FDR] <0.01) between subjects with or without BCAR, from which linear discriminant analysis and cross-validation identified an initial gene signature of 24 probe sets, and a more refined set of 11 probe sets found to classify subject samples correctly. Cross-validation suggested an out-of-sample sensitivity of 73% and specificity of 91% for identification of samples with or without BCAR. An increase in classifier gene expression correlated closely with acute rejection during the first 3 months posttransplant. Biological evaluation indicated that the differentially expressed genes encompassed processes related to immune response, signal transduction, and cytoskeletal reorganization.

CONCLUSION

Preliminary evidence indicates that gene expression in the peripheral blood may yield a relevant measure for the occurrence of BCAR and offer a potential tool for immunologic monitoring. These results now require confirmation in a larger cohort.

摘要

背景

急性移植物排斥是肾移植中的一个重要临床问题,也是长期移植物存活的不良预测因子。提供早期移植物排斥证据的外周血生物标志物可为移植后监测提供重要选择,优化移植活检的实用性,并允许及时进行有效的治疗干预,以最小化移植物损伤。

方法

在这项可行性研究(n=58)中,我们使用病例对照设计中的基因表达谱分析比较了正常受试者(n=20)与经活检证实的急性排斥(BCAR)(n=11)或无 BCAR(n=22)或边界改变(n=5)患者的全血样本。

结果

共有 183 个探针集(代表 160 个基因)在有无 BCAR 的受试者之间表达差异(错误发现率[FDR] <0.01),线性判别分析和交叉验证确定了最初的 24 个探针集基因特征,以及更精细的 11 个探针集可正确分类受试者样本。交叉验证表明,用于识别有无 BCAR 样本的样本外灵敏度为 73%,特异性为 91%。分类器基因表达的增加与移植后前 3 个月的急性排斥密切相关。生物学评估表明,差异表达的基因包含与免疫反应、信号转导和细胞骨架重排相关的过程。

结论

初步证据表明,外周血中的基因表达可能提供与 BCAR 发生相关的相关测量,并为免疫监测提供潜在工具。这些结果现在需要在更大的队列中得到证实。

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