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构建心脏移植排斥反应的基于组织的分子诊断系统:心脏分子显微镜诊断(MMDx)系统。

Building a tissue-based molecular diagnostic system in heart transplant rejection: The heart Molecular Microscope Diagnostic (MMDx) System.

机构信息

Alberta Transplant Applied Genomics Centre, Edmonton, Alberta, Canada; Division of Nephrology and Transplant Immunology, Department of Medicine, University of Alberta, Edmonton, Alberta, Canada.

Cardiovascular Department, University of Bologna, Bologna, Italy.

出版信息

J Heart Lung Transplant. 2017 Nov;36(11):1192-1200. doi: 10.1016/j.healun.2017.05.029. Epub 2017 May 29.

Abstract

BACKGROUND

The emergence of molecular systems offers opportunities for improving the assessment of rejection in heart transplant biopsy specimens. The present study developed a microarray-based system for assessing heart transplant endomyocardial biopsy (EMB) specimens.

METHODS

We analyzed 331 protocol or for-cause EMB specimens from 221 subjects in 3 centers (Edmonton, Bologna, and Paris). Unsupervised principal component analysis (PCA) and archetype analysis used rejection-associated transcripts (RATs) shown in kidney transplants to be associated with antibody-mediated rejection (ABMR) or T cell-mediated rejection (TCMR), or both. To compare EMB specimens to kidney biopsy specimens, rejection status in both was simplified to TCMR, ABMR, or no rejection.

RESULTS

The pattern of RAT expression was similar in EMB and kidney specimens, permitting use of RATs to assign scores and group ("cluster") membership to each EMB, independent of histology. Three clusters emerged in EMB specimens, similar to kidney specimens: TCMR, ABMR, and no rejection. This permitted each EMB specimen to be given 3 scores and assigned to 1 cluster by its highest score. There was significant agreement between molecular phenotype-archetype scores or clusters-and both histologic diagnoses and donor-specific antibody. Area under curve estimates for predicting histologic TCMR, ABMR, and no rejection by molecular assessment were lower in EMB specimens than in kidney specimens, reflecting more uncertainty in EMB specimens, particularly in histologic diagnosis of TCMR.

CONCLUSIONS

Rejection-associated transcripts can be used to estimate the probability of TCMR and ABMR in heart transplant specimens, providing a new dimension to improve the accuracy of diagnoses and an independent system for recalibrating the histology guidelines.

摘要

背景

分子系统的出现为改善心脏移植活检标本排斥反应的评估提供了机会。本研究开发了一种基于微阵列的系统来评估心脏移植心内膜活检(EMB)标本。

方法

我们分析了来自 3 个中心(埃德蒙顿、博洛尼亚和巴黎)的 221 名患者的 331 例方案或因原因的 EMB 标本。未监督的主成分分析(PCA)和原型分析使用与肾移植中抗体介导的排斥反应(ABMR)或 T 细胞介导的排斥反应(TCMR)相关的排斥相关转录物(RAT),或两者都有。为了将 EMB 标本与肾活检标本进行比较,简化了两者的排斥状态,分为 TCMR、ABMR 或无排斥。

结果

EMB 和肾标本中 RAT 表达模式相似,允许使用 RAT 为每个 EMB 分配评分和组(“聚类”)成员,而不依赖于组织学。EMB 标本中出现了 3 个聚类,与肾标本相似:TCMR、ABMR 和无排斥。这允许每个 EMB 标本获得 3 个评分,并根据其最高评分分配给 1 个聚类。分子表型-原型评分或聚类与组织学诊断和供体特异性抗体之间存在显著一致性。通过分子评估预测组织学 TCMR、ABMR 和无排斥的曲线下面积估计值在 EMB 标本中低于肾标本,这反映了 EMB 标本中的不确定性更大,特别是在 TCMR 的组织学诊断中。

结论

排斥相关转录物可用于估计心脏移植标本中 TCMR 和 ABMR 的概率,为提高诊断准确性提供了新的维度,并为重新校准组织学指南提供了独立的系统。

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