一项在被诊断为小缺血性中风或中风模拟患者的急性期外周血基因表达的病例对照比较。
A case-control comparison of acute-phase peripheral blood gene expression in participants diagnosed with minor ischaemic stroke or stroke mimics.
机构信息
Queensland Research Centre for Peripheral Vascular Disease, College of Medicine and Dentistry, James Cook University, Townsville, QLD, 4811, Australia.
Australian Institute of Tropical Health and Medicine, James Cook University, Townsville, QLD, 4811, Australia.
出版信息
Hum Genomics. 2023 Nov 25;17(1):106. doi: 10.1186/s40246-023-00551-y.
BACKGROUND
Past studies suggest that there are changes in peripheral blood cell gene expression in response to ischaemic stroke; however, the specific changes which occur during the acute phase are poorly characterised. The current study aimed to identify peripheral blood cell genes specifically associated with the early response to ischaemic stroke using whole blood samples collected from participants diagnosed with ischaemic stroke (n = 29) or stroke mimics (n = 27) following emergency presentation to hospital. Long non-coding RNA (lncRNA), mRNA and micro-RNA (miRNA) abundance was measured by RNA-seq, and the consensusDE package was used to identify genes which were differentially expressed between groups. A sensitivity analysis excluding two participants with metastatic disease was also conducted.
RESULTS
The mean time from symptom onset to blood collection was 2.6 h. Most strokes were mild (median NIH stroke scale score 2.0). Ten mRNAs (all down-regulated in samples provided by patients experiencing ischaemic stroke) and 30 miRNAs (14 over-expressed and 16 under-expressed in participants with ischaemic stroke) were significantly different between groups in the whole cohort and sensitivity analyses. No significant over-representation of gene ontology categories by the differentially expressed genes was observed. Random forest analysis suggested a panel of differentially expressed genes (ADGRG7 and miRNAs 96, 532, 6766, 6798 and 6804) as potential ischaemic stroke biomarkers, although modelling analyses demonstrated that these genes had poor diagnostic performance.
CONCLUSIONS
This study provides evidence suggesting that the early response to minor ischaemic stroke is predominantly reflected by changes in the expression of miRNAs in peripheral blood cells. Further work in independent cohorts particularly in patients with more severe stroke is needed to validate these findings and investigate their clinical relevance.
背景
过去的研究表明,外周血细胞基因表达会发生变化,以应对缺血性中风;然而,急性期中发生的确切变化尚不清楚。本研究旨在使用从因疑似缺血性中风(n=29)或中风模拟症(n=27)而在医院急诊就诊的患者中采集的全血样本,鉴定与缺血性中风早期反应相关的特定外周血细胞基因。通过 RNA-seq 测量长链非编码 RNA(lncRNA)、mRNA 和 microRNA(miRNA)的丰度,并使用共识 DE 包鉴定组间差异表达的基因。还进行了一项敏感性分析,排除了两名患有转移性疾病的患者。
结果
从症状发作到采血的平均时间为 2.6 小时。大多数中风为轻度(中位数 NIH 中风量表评分为 2.0)。在整个队列和敏感性分析中,10 个 mRNA(在经历缺血性中风的患者样本中均下调)和 30 个 miRNA(14 个在缺血性中风患者中上调,16 个下调)在组间存在显著差异。差异表达基因没有明显的基因本体类别过度表达。随机森林分析表明,一组差异表达基因(ADGRG7 和 miRNA 96、532、6766、6798 和 6804)可能作为潜在的缺血性中风生物标志物,尽管建模分析表明这些基因的诊断性能较差。
结论
本研究提供的证据表明,轻微缺血性中风的早期反应主要反映在外周血单个核细胞中 miRNA 的表达变化。需要在独立队列中进行进一步的工作,特别是在中风更严重的患者中,以验证这些发现并研究其临床相关性。
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