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猪到灵长类动物异位异种移植后心脏基因表达的变化。

Changes in cardiac gene expression after pig-to-primate orthotopic xenotransplantation.

机构信息

Department of Medicine, University College London, London, UK.

出版信息

Xenotransplantation. 2011 Jan-Feb;18(1):14-27. doi: 10.1111/j.1399-3089.2010.00620.x.

Abstract

BACKGROUND

Gene profiling methods have been widely useful for delineating changes in gene expression as an approach for gaining insight into the mechanism of rejection or disease pathology. Herein, we use gene profiling to compare changes in gene expression associated with different orthotopic cardiac xenotransplantation (OCXTx) outcomes and to identify potential effects of OCXTx on cardiac physiology.

METHODS

We used the Affymetrix GeneChip Porcine Genomic Array to characterize three types of orthotopic cardiac xenograft outcomes: 1) rejected hearts that underwent delayed xenograft rejection (DXR); 2) survivor hearts in which the xenograft was not rejected and recipient death was due to model complications; and 3) hearts which failed to provide sufficient circulatory support within the first 48 h of transplant, termed "perioperative cardiac xenograft dysfunction" (PCXD). Gene expression in each group was compared to control, not transplanted pig hearts, and changes in gene expression > 3 standard deviations (±3SD) from the control samples were analyzed. A bioinformatics analysis was used to identify enrichments in genes involved in Kyoto Encyclopedia of Genes and Genomes pathways and gene ontogeny molecular functions. Changes in gene expression were confirmed by quantitative RT-PCR.

RESULTS

The ±3SD data set contained 260 probes, which minimally exhibited a 3.5-fold change in gene expression compared to control pig hearts. Hierarchical cluster analysis segregated rejected, survivor and PCXD samples, indicating a unique change in gene expression for each group. All transplant outcomes shared a set of 21 probes with similarly altered expression, which were indicative of ongoing myocardial inflammation and injury. Some outcome-specific changes in gene expression were identified. Bioinformatics analysis detected an enrichment of genes involved in protein, carbohydrate and branched amino acid metabolism, extracellular matrix-receptor interactions, focal adhesion, and cell communication.

CONCLUSIONS

This is the first genome wide assessment of changes in cardiac gene expression after OCXTx. Hierarchical cluster analysis indicates a unique gene profile for each transplant outcome but additional samples will be required to define the unique classifier probe sets. Quantitative RT-PCR confirmed that all transplants exhibited strong evidence of ongoing inflammation and myocardial injury consistent with the effects of cytokines and vascular antibody-mediated inflammation. This was also consistent with bioinformatic analysis suggesting ongoing tissue repair in survivor and PCXD samples. Bioinformatics analysis suggests for the first time that xenotransplantation may affect cardiac metabolism in survivor and rejected samples. This study highlights the potential utility of molecular analysis to monitor xenograft function, to identify new molecular markers and to understand processes, which may contribute to DXR.

摘要

背景

基因谱分析方法已广泛用于描绘基因表达的变化,以此作为深入了解排斥反应或疾病发病机制的一种方法。在此,我们使用基因谱分析比较不同同种异体心脏移植(OCXTx)结果相关的基因表达变化,并确定 OCXTx 对心脏生理学的潜在影响。

方法

我们使用 Affymetrix GeneChip Porcine Genomic Array 来描述三种类型的同种异体心脏移植结果:1)经历延迟异种移植物排斥(DXR)的排斥心脏;2)异种移植物未被排斥且受体因模型并发症而死亡的存活心脏;3)在移植后的前 48 小时内未能提供足够的循环支持的心脏,称为“围手术期心脏异种移植功能障碍”(PCXD)。每组的基因表达与未移植的猪心进行比较,分析基因表达变化大于对照样本 3 个标准差(±3SD)的基因。使用生物信息学分析鉴定京都基因与基因组百科全书(KEGG)途径和基因本体论(GO)分子功能中涉及的基因富集。通过定量 RT-PCR 确认基因表达的变化。

结果

±3SD 数据集包含 260 个探针,与对照猪心相比,这些探针的基因表达至少有 3.5 倍的变化。层次聚类分析将排斥、存活和 PCXD 样本分开,表明每个组的基因表达都有独特的变化。所有移植结果都有一组 21 个探针的表达相似,这表明存在持续的心肌炎症和损伤。确定了一些与结果相关的基因表达变化。生物信息学分析检测到参与蛋白质、碳水化合物和支链氨基酸代谢、细胞外基质-受体相互作用、焦点粘连和细胞通讯的基因富集。

结论

这是首次对 OCXTx 后心脏基因表达变化进行全基因组评估。层次聚类分析表明每个移植结果都有独特的基因谱,但需要更多的样本来定义独特的分类探针集。定量 RT-PCR 证实所有移植均表现出强烈的持续炎症和心肌损伤证据,这与细胞因子和血管抗体介导的炎症的影响一致。这也与生物信息学分析一致,表明存活和 PCXD 样本中持续存在组织修复。生物信息学分析首次表明异种移植可能影响存活和排斥样本的心脏代谢。本研究强调了分子分析在监测异种移植物功能、识别新的分子标记以及了解可能导致 DXR 的过程方面的潜在用途。

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