Nopp Stephan, Königsbrügge Oliver, Schmaldienst Sabine, Säemann Marcus, Pabinger Ingrid, Nossent Anne Yaël, Ay Cihan
Division of Hematology and Hemostaseology, Department of Medicine I, Medical University of Vienna, Vienna, Austria.
Department of Medicine I, Clinic Favoriten, Vienna, Austria.
Thromb Haemost. 2025 Jul;125(7):674-685. doi: 10.1055/a-2413-2792. Epub 2024 Sep 11.
Patients with end-stage kidney disease (ESKD) are at very high risk for thromboembolism and bleeding. This study aimed to identify small noncoding RNAs (sncRNAs), specifically microRNAs and transfer-RNA (tRNA)-derived fragments (tRFs), as potential novel biomarkers for predicting thromboembolism and bleeding in this high-risk population.
In this sncRNA discovery research, we leveraged the VIVALDI cohort, consisting of 625 ESKD patients on hemodialysis, to conduct two nested case-control studies, each comprising 18 participants. The primary outcomes were ischemic stroke in the first study and major bleeding in the second. Plasma samples were processed using the miND pipeline for RNA-seq analysis to investigate differential expression of microRNAs and tRNA/tRFs between cases and their respective matched controls, with results stringently adjusted for the false discovery rate (FDR).
No significant differential expression of microRNAs for either ischemic stroke or major bleeding outcomes was observed in the two nested case-control studies. However, we identified four tRNAs significantly differentially expressed in ischemic stroke cases and seven in major bleeding cases, compared with controls (FDR < 0.1). Coverage plots indicated that specific tRNA fragments (tRFs), rather than full-length tRNAs, were detected, however. Alternative mapping approaches revealed challenges and technical limitations that precluded in-depth differential expression analyses on these specific tRFs. Yet, they also underscored the potential of tRNAs and tRFs as markers for thromboembolism and bleeding.
While microRNAs did not show significant differential expression, our study identifies specific tRNAs/tRFs as potential novel biomarkers for ischemic stroke and major bleeding in ESKD patients.
终末期肾病(ESKD)患者发生血栓栓塞和出血的风险非常高。本研究旨在鉴定小非编码RNA(sncRNAs),特别是微小RNA和转移RNA(tRNA)衍生片段(tRFs),作为预测这一高危人群血栓栓塞和出血的潜在新型生物标志物。
在这项sncRNA发现研究中,我们利用了由625例接受血液透析的ESKD患者组成的VIVALDI队列,进行了两项嵌套病例对照研究,每项研究包括18名参与者。第一项研究的主要结局是缺血性中风,第二项研究的主要结局是大出血。血浆样本使用miND流程进行处理,以进行RNA测序分析,研究病例与其各自匹配对照之间微小RNA和tRNA/tRFs的差异表达,并对结果进行严格的错误发现率(FDR)校正。
在两项嵌套病例对照研究中,未观察到微小RNA在缺血性中风或大出血结局方面有显著差异表达。然而,与对照组相比,我们发现有4种tRNA在缺血性中风病例中显著差异表达,7种在大出血病例中显著差异表达(FDR<0.1)。覆盖图表明,检测到的是特定的tRNA片段(tRFs),而非全长tRNA。替代映射方法揭示了一些挑战和技术限制,这些限制妨碍了对这些特定tRFs进行深入的差异表达分析。然而,它们也强调了tRNA和tRFs作为血栓栓塞和出血标志物的潜力。
虽然微小RNA未显示出显著差异表达,但我们的研究确定了特定的tRNA/tRFs作为ESKD患者缺血性中风和大出血的潜在新型生物标志物。
