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心房颤动的转录图谱:一项系统综述和荟萃分析。

The transcriptional landscape of atrial fibrillation: A systematic review and meta-analysis.

作者信息

Gómez-Ochoa Sergio Alejandro, Möhn Malte, Malz Michelle Victoria, Ottenheijm Roger, Lanzer Jan D, Wiedmann Felix, Kraft Manuel, Muka Taulant, Schmidt Constanze, Freichel Marc, Levinson Rebecca T

机构信息

Department of General Internal Medicine and Psychosomatics, Heidelberg University Hospital, University of Heidelberg, Heidelberg, Germany.

Institute for Computational Biomedicine, Heidelberg University Faculty of Medicine, Heidelberg University Hospital, University of Heidelberg, Heidelberg, Germany.

出版信息

PLoS One. 2025 May 30;20(5):e0323534. doi: 10.1371/journal.pone.0323534. eCollection 2025.

Abstract

BACKGROUND

Despite advances in understanding atrial fibrillation (AF) pathophysiology, there is limited agreement on the key genes driving its pathophysiology. To understand the genome-wide transcriptomic landscape, we performed a meta-analysis from studies reporting gene expression patterns in atrial heart tissue from patients with AF and controls in sinus rhythm (SR).

METHODS

Bibliographic databases and data repositories were systematically searched for studies reporting gene expression patterns in atrial heart auricle tissue from patients with AF and controls in sinus rhythm. We calculated the pooled differences in individual gene expression from fourteen studies comprising 534 samples (353 AF and 181 SR) to create a consensus signature (CS), from which we identified differentially regulated pathways, estimated transcription factor activity, and evaluated its performance in classifying validation samples as AF or SR.

RESULTS

Despite heterogeneity in the top differentially expressed genes across studies, the AF-CS in both chambers were robust, showing a better performance in classifying AF status than individual study signatures. Functional analysis revealed commonality in the dysregulated cellular processes between chambers, including extracellular matrix remodeling (highlighting epithelial mesenchymal transition, actin filament organization, and actin binding hallmark pathways), cardiac conduction (including cardiac muscle cell action potential, gated channel activity, and cation channel activity pathways), metabolic derangements (highlighting oxidative phosphorylation and asparagine n linked glycosylation), and innate immune system activity (mainly neutrophil degranulation, and TNFα signaling pathways). Finally, the AF-CS showed a good performance differentiating AF from controls in three validation datasets (two from peripheral blood and one from left ventricle samples).

CONCLUSIONS

Despite variability in individual studies, this meta-analysis elucidated conserved molecular pathways involved in AF pathophysiology across its phenotypes and the potential of a transcriptomic signature in identifying AF from peripheral blood samples. Our work highlights the value of integrating published transcriptomics data in AF and the need for better data deposition practices.

摘要

背景

尽管在理解心房颤动(AF)的病理生理学方面取得了进展,但对于驱动其病理生理学的关键基因,人们的共识有限。为了了解全基因组转录组情况,我们对报告房颤患者和窦性心律(SR)对照者心房组织基因表达模式的研究进行了荟萃分析。

方法

系统检索文献数据库和数据储存库,以查找报告房颤患者和窦性心律对照者心房心耳组织基因表达模式的研究。我们计算了来自14项研究(共534个样本,353个房颤样本和181个SR样本)的个体基因表达的合并差异,以创建一个共识特征(CS),从中我们识别出差异调节的通路,估计转录因子活性,并评估其在将验证样本分类为房颤或SR方面的性能。

结果

尽管各研究中差异表达最显著的基因存在异质性,但两个心房的房颤-CS都很稳健,在分类房颤状态方面比单个研究特征表现更好。功能分析揭示了两个心房之间失调的细胞过程的共性,包括细胞外基质重塑(突出上皮-间质转化、肌动蛋白丝组织和肌动蛋白结合标志性通路)、心脏传导(包括心肌细胞动作电位、门控通道活性和阳离子通道活性通路)、代谢紊乱(突出氧化磷酸化和天冬酰胺N-连接糖基化)以及先天免疫系统活性(主要是中性粒细胞脱颗粒和TNFα信号通路)。最后,房颤-CS在三个验证数据集(两个来自外周血,一个来自左心室样本)中表现出良好的区分房颤与对照的性能。

结论

尽管个体研究存在差异,但这项荟萃分析阐明了房颤病理生理学中跨其表型的保守分子通路以及转录组特征从外周血样本中识别房颤的潜力。我们的工作强调了整合已发表的房颤转录组学数据的价值以及更好的数据存档做法的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4776/12124854/72daef1b1837/pone.0323534.g001.jpg

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